WO2011069094A1 - Methods of administering pirfenidone therapy - Google Patents

Abstract

The present invention relates to methods involving avoiding adverse drug interactions with fluvoxamine and pirfenidone or other moderate to strong inhibitors of CYP enzymes.

Description

METHODS OF ADMINISTERING PI R I- M DON E THERAPY

FIELD OF THE INVENTION

[0001 ] The invention relates to improved methods of administering pirfenidone therapy involving avoiding adverse drug interactions with fJuvoxamine, a strong inhibitor of CYP1A2.

BACKGROUND

[0002] Pirfenidone is small molecule with a molecular weight of 185.23 daltons whose chemical name is 5-methyl-l -phenyl-2-(l H)-pyridone. Pirfenidone has anti-fibrotic properties and has been investigated for therapeutic benefits to patients suffering from various fibrotic conditions. It is approved in Japan for treatment of idiopathic pulmonary fibrosis (IPF) under the trade name Pirespa®.

[0003] Pirfenidone has been shown to be metabolized by various isoforms of the cytochrome P450 (CYP) protein [See the Report on the Deliberation Results, Evaluation and Licensing Division, Phannaceuticai and Food Safety Bureau, Ministry of Health Labour and Welfare, September 16, 2008]. Specifically, several cytochrome P450 (CYP) isoforms (CYP1 A2, 2C9, 2C 19, 2D6 and 2E1 ) were involved in the earliest stages of oxidative metabolism of pirfenidone.

[0004] Fluvoxamine belongs to a class of therapeutics known as selective serotonin reuptake inhibitors (SSRIs). The SSRIs are a group of antidepressants with similar pharmacologic effects, but with different chemical structures. Fluvoxamine has been approved for treatment of social anxiety disorder (social phobia), obsessive compulsive disorder (OCD), and has been prescribed to treat major depression, and other anxiety disorders such as panic disorder and post-traumatic stress disorder [McClellan et al., (Drugs October 2000). "Fluvoxamine An Updated Review of its Use in the Management of Adults with Anxiety Disorders". Adis Drug Evaluation 60 (4): 925-954]. In addition to

fluvoxamine, other clinically available SSRIs are citalopram, fluoxetine, paroxetine and sertraline. The elimination of these lipophilic compounds proceeds predominantly via oxidation catalysed by CYP in the li ver. SSRIs have the potential for inhibition of CYP enzymes [Brosen, The pharmacogenetics of the selective serotonin reuptake inhibitors. Clin Invest 71 ( 12): 1002-1009, 1993]. Jeppesen et al. reported that fluvoxamine is a potent inhibitor of CYP1A2 in humans in vivo [Jeppesen et al. , Dose-dependent inhibition of CYP1 A2, CYP2C19 and CYP2D6 by citalopram, fluoxetine, fluvoxamine and paroxetine. Eur J Clin Pharmacol 51 : 73-78, 1996]. Fluvoxamine has also been shown to be a very potent inhibitor of CYP1A2 in vitro [Broscn et al , Fluvoxamine is a potent inhibitor of cytochrome P4501A2. Biochem Pharmacol 45: 121 1-1214, 1993; Rasmussen et al , Selective serotonin reuptake inhibitors and theophylline metabolism in human liver microsomes: potent inhibition by fluvoxamine. Br J Clin Pharmacol 39: 151 -159, 1995].

SUMMARY OF THE INVENTION

[0005J The invention disclosed herein is based on the discovery of an adverse drug interaction between pirfenidone and fluvoxamine.

[0006J The invention generally relates to improved uses and methods of administering pirfenidone to a patient in need of pirfenidone therapy, and to methods of preparing or packaging pirfenidone medicaments, containers, packages and kits. In any of the aspects or embodiments, the patient may have idiopathic pulmonary fibrosis (IPF) and the medicament is for treatment of IPF. In any of the aspects or embodiments, the therapeutically effective amount of pirfenidone being administered may be a daily dosage of 2400 mg or 2403 mg per day. In any of the aspects of the invention, the daily dosage may be administered in divided doses three times a day, or two times a day, or alternatively is administered in a single dose once a day. In any of the aspects of the invention, the pirfenidone may be administered with food. For example, the daily dosage of 2400 mg or 2403 mg pirfenidone per day may be administered as follows: 801 mg taken three times a day, with food.

[0007] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy (e.g. , a patient with IPF), involving administering to the patient a therapeutically effective amount of pirfenidone, and avoiding administration of fluvoxamine despite the patient being in need of fluvoxamine therapy.

[0008 J In other aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy, comprising discontinuing administration of fluvoxamine to avoid an adverse drug interaction and administering a therapeutically effective amount of pirfenidone. In one embodiment, the patient is in need of and thus is receiv ing fluvoxamine, and fluvoxamine is discontinued concurrent with starting

administration of pirfenidone. In another embodiment, fluvoxamine is discontinued within at least 3 days to 1 month prior to or after starting pirfenidone therapy. This time period, for example, permits adequate time for tapering and withdrawal without adverse effects. In one example, in a method of administering a therapeutically effective amount o pirfenidone to a patient with 1PF, the invention provides an improvement that comprises avoiding or discontinuing administration of fluvoxamine and administering a therapeutically effective amount of pirfenidone.

[00091 As used herein, an adverse drug interaction can include reduced clearance of pirfenidone, the potential for reduced clearance of pirfenidone, increased exposure to pirfenidone, or the potential for increased exposure to pirfenidone.

[001 OJ Thus, an aspect of the invention provides pirfenidone for use in treating a patient in need of pirfenidone therapy, characterized in that the treating comprises avoiding, contraindicating or discontinuing concomitant use (or co-administration) of fluvoxamine. In some embodiments, the concomitant use of fluvoxamine is avoided, contraindicated or discontinued, in order to avoid reduced clearance of pirfenidone, or the potential for reduced clearance of pirfenidone. In some embodiments, the concomitant use of fluvoxamine is avoided, contraindicated or discontinued, in order to avoid increased exposure to pirfenidone, or the potential for increased exposure to pirfenidone. Administration of pirfenidone in patients that concomitantly use or are being administered fluvoxamine results in about a 6- fold increase in pirfenidone exposure. It is understood that any of the aspects or

embodiments or examples described herein with respect to methods of treatment apply to this aspect of the invention that provides pirfenidone for use in treating a patient. For example, the patient may be a patient with IPF, and the therapeutically effective amount administered may be 2400 or 2403 tng per day.

[0011 ] Similarly, a further aspect of the invention provides the use of pirfenidone in the manufacture of a medicament for treating a patient in need of pirfenidone therapy, characterized in that the treating comprises avoiding, contraindicating or discontinuing concomitant use (or co-administration) o fluvoxamine. It is understood that any of the aspects or embodiments or examples described herein with respect to methods of treatment or "pirfenidone for use" in treating a patient apply to this aspect of the invention that provides for the use of pirfenidone in manufacture of a medicament. For example, the patient may be a patient with IPF, and the therapeutical ly effective amount administered may be 2400 or 2403 mg per day.

[0012] As used herein, "concomitant use" is understood to be interchangeable with concurrent administration or co-administration. Thus, the terms are understood to encompass administration simultaneously . or at different times, and by the same route or by di fferent routes, as long as the two agents are given in a manner that allows both agents to be affecting the body at the same time. For example, concomitant use can refer to a medication concomitantly administered, whether prescribed by the same or a different practitioner, or for the same or a different indication.

[0013] In some embodiments, the patient is a patient in need of therapy with a CYP 1A2 inhibitor. In some embodiments, the patient is a patient in need of therapy with a strong CYP 1 A2 inhibitor, or a moderate to strong CYP 1 A2 inhibitor. In some embodiments, the patient is a patient in need of fluvoxamine therapy. In some embodiments, the patient is a patient who is avoiding concomitant use of fluvoxamine, e.g. because concomitant use of pirfenidone with fluvoxamine is contraindicated. In some embodiments, the patient is a patient who was or is being administered a strong CYP 1A2 inhibitor, or a moderate to strong CYP 1 A2 inhibitor, e.g. fluvoxamine. In some embodiments, the patient is a patient who has discontinued use of a strong CYP 1 A2 inhibitor, or a moderate to strong CYP 1 A2 inhibitor prior to the initiation of pirfenidone therapy in order to avoid reduced clearance (or increased exposure to) pirfenidone, or the potential for reduced clearance of (or increased exposure to) pirfenidone. In some embodiments, the patient is a patient who has discontinued use of fluvoxamine prior to the initiation of pirfenidone therapy in order to avoid reduced clearance of pirfenidone, or the potential for reduced clearance of pirfenidone. In some embodiments, the patient is a patient who has discontinued use of fluvoxamine prior to the initiation of pirfenidone therapy in order to avoid increased exposure to pirfenidone. or the potential for increased exposure to pirfenidone. In some embodiments, the patient is a patient who has discontinued administration of the strong CYP 1 A2 inhibitor, or moderate to strong CYP1 A2 inhibitor, e.g., fluvoxamine, within 1 month, or within 2 weeks, prior to starting pirfenidone therapy, or concurrent with starting pirfenidone therapy. It is understood that any of the aspects or embodiments or examples described herein with respect to methods of treatment apply to this aspect of the invention that provides for characterization o f the patients to be treated with pirfenidone.

[0014] In yet other aspects, a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy and in need o f fluvoxamine therapy is provided, comprising administering a therapeutically effective amount of pirfenidone to the patient, and

administeri ng an alternative therapy that is not fluvoxamine. In one aspect, the alternative therapy that i s not fluvoxamine is a drug that is not a strong or moderate to strong inhibitor of cytochrome P450 1 A2 (CYP 1 A2). Pre ferabl y, such drug is not a moderate to strong inhibitor of both CY P 1 A2, and another CYP en/ymc selected from the group consisting of CYP3A4, CYP2C9, and/or CYP2C19. In some examples, the alternative drug is selected from the group consisting of Citalopram (Celexa), Escitalopram (Lexapro), Fluoxetine (Prozac, Prozac Weekly), Paroxetine (Paxil, Paxil CR, Pexeva), and/or Sertraline (Zoloft) .

[0015] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy (e.g. , a patient with IPF), involving administering to the patient a therapeutically effective amount of pirfenidone, and advising the patient in any one, two, three or more of the following ways:

(a) advising the patient that fluvoxamine should be avoided or discontinued,

(b) advising the patient that co-administration of pirfenidone with drugs that are moderate to strong inhibitors of both CYPl A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, and/or CYP2C19. , can alter the therapeutic effect or adverse reaction profile of pirfenidone,

(c) advising the patient that co-administration of pirfenidone with fluvoxamine can alter the therapeutic effect or adverse reaction profile of pirfenidone,

(d) advising the patient that use of pirfenidone in patients being treated with fluvoxamine is contraindicated,

(e) advising the patient that co-administration of pirfenidone and fluvoxamine resulted in an average 6- fold increase in exposure to pirfenidone, and/or.

(f) advising the patient that strong CYPl A2 inhibitors should be used with caution in patients receiving pirfenidone due to the potential for reduced pirfenidone clearance.

[0016] In some embodiments, the method further includes advising the patient that coadministration of pirfenidone and fluvoxamine resulted in a 2-fold increase in average peak serum concentration of pirfenidone (Cmax ). In yet further embodiments, the method also includes avoiding administering a strong CYPl A2 inhibitor, or discontinuing administration of a strong CYP 1 A2 inhibitor.

[0017] In some embodiments, a method of reducing toxicity of pirfenidone treatment in a patient is provided comprising administering a therapeutically effective amount of pirfenidone to the patient and advising the patient of any of the foregoing advice.

[0018| In some embodiments, a method of improving safety of pirfenidone treatment in a patient is provided comprising administering a therapeutically effective amount of pirfenidone to the patient and advising the patient of any of the foregoing advice. 10019] In some embodiments, a method of reducing adverse drug interaction with pirfenidone treatment in a patient is provided comprising administering a therapeutically effective amount of pirfenidone to the patient and advising the patient of any of the foregoing advice.

[0020] Thus, in some embodiments, the concomitant use of fluvoxamine is avoided, contraindicated or discontinued in order to:

(a) avoid altering the therapeutic effect profile of pirfenidone, and/or

(b) avoid altering the adverse reaction profile of pirfenidone, and/or

(c) avoid the increased exposure or potential for increased exposure, and/or

(d) avoid the reduced clearance or potential for reduced clearance, and/or

(e) avoid the average 6-fold increase in exposure to pirfenidone upon concomitant administration with fluvoxamine, and/or

(f) avoid the average 2-fold increase in average peak serum concentration of pirfenidone (Cmax) upon concomitant administration with fluvoxamine, and/or

(g) reduce toxicity of pirfenidone treatment, and/or

(h) improve safety of pirfenidone treatment, and/or

(i) reduce adverse drug interaction associated with pirfenidone treatment.

BRIEF DESCRIPTION OF THE DRAWING

[0021 ] Figure 1 depicts a symmetrical dot plot of AUCo_-∞ estimates by study day— circles indicate smokers, triangles indicate nonsmokers.

DETAILED DESCRIPTION OF THE INVENTION

[0022] Pirfenidone is an orally active, anti-fibrotic agent. Results of in vitro experiments indicated that pirfenidone is primarily metabolized by CYP1 A2 (approx. 48" ;.) with multiple other CYPs contributing as well (each <13%) (i.e., 1 A 1 , 2A6, 2B6, 2C8, 2C , 2C18, 2C 19, 2D6, 2E1. 212, 3A4, 3A5, 4A1 1. and 41· 2 ). Oral administration of pirfenidone results in the formation of four metabolites, 5 hydroxymeihyl-pirfenidone, 5 carboxy-pirfenidone, 4'- hydroxy-pirfeuidone, and the 5 O-acyl glucuronide metabolite of 5 carboxy-pirfenidone. In humans, only pirfenidone and 5-carboxy-pirfenidone are present in plasma in significant quantities; none of the other metabolites occur in sufficient quantities to allow for PK analysis. There are no unique human metabolites.

[0023] Fluvoxamine is a potent CYP 1 A2 and CYP2C 19 inhibitor, and a moderate CYP2C9, CYP2D6, and CYP3A4 inhibitor [Hemeryck et al , Selective Serotonin Reuptake Inhibitors and Cytochrome P-450 Mediated Drug-Drug Interactions: An Update. Current Drug Metabolism 3(1): 1 3-37, 2002] .

[0024] The invention disclosed herein is based on the discovery of an adverse drug interaction between pirfenidone and fluvoxamine. Adverse dmg interactions represent 3-5% of preventable in-hospital adverse drug reactions, and are an important contributor to the number of emergency room visits and hospital admissions [Leape LL et al , JAMA

1995;274( 1 ):35 -43; Raschetti R et al. Eur J Clin Pharmacol 1999;54( 12):959-963] .

[0025] Data reported herein show that co-administration of pirfenidone with fluvoxamine resulted in an average 6-fold increase in exposure (AUC, or area under the curve) to pirfenidone. It also resulted in an average 2-fold increase in Cmax, the mean maximum plasma concentration. Depending on the circumstances, FDA draft guidance suggests that a drug-drug interaction is present when comparisons indicate twofold or greater systemic exposure for a drug when given in combination with the second drug, compared to when given alone. FDA Preliminary Concept Paper, "Drug Interaction Studies - Study Design, Data Analysis, and Implications for Dosing and Labeling," October 1 , 2004.

Definitions

[0026] The terms "therapeutically effective amount," as used herein, refer to an amount of a compound sufficient to treat, ameliorate, or prevent the identified disease or condition, or to exhibit a detectable therapeutic, prophylactic, or inhibitory effect. The effect can be detected by, for example, an improvement in clinical condition, or reduction in symptoms. The precise effective amount for a subject will depend upon the subject's body weight, size, and health; the nature and extent of the condition; and the therapeutic or combination of therapeutics selected for administration. Where a drug has been approved by the U.S. Food and Drug Admini stration (FDA), a "therapeutical ly effective amount" refers to the dosage approved by the FDA or its counterpart foreign agency for treatment of the identified disease or condition.

[0027] As used herein, a patient "in need of pirfenidone therapy" is a patient who would benefit from administration of pirfenidone. The patient may be suffering from any disease or condition f r w hich pirfenidone therapy may be useful in ameliorating symptoms. Such diseases or conditions include pulmonary fibrosis, idiopathic pulmonary fibrosis, idiopathic interstitial pneumonia, autoimmune lung diseases, benign prostate hypertrophy, coronary or myocardial infarction, atrial fibrillation, cerebral infarction, myocardiac fibrosis,

musculoskeletal fibrosis, post-surgical adhesions, liver cirrhosis, renal fibrotic disease, fibrotic vascular disease, scleroderma, Herman sky-Pudlak syndrome, neurofibromatosis, Alzheimer's disease, diabetic retinopathy, and/or skin lesions, lymph node fibrosis associated with HIV, chronic obstructive pulmonary disease (COPD), inflammatory pulmonary fibrosis, rheumatoid arthritis; rheumatoid spondylitis; osteoarthritis; gout, other arthritic conditions; sepsis; septic shock; endotoxic shock; gram-negative sepsis; toxic shock syndrome;

myofacial pain syndrome (MPS); Shigellosis; asthma; adult respiratory distress syndrome; inflammatory bowel disease; Crohn's disease; psoriasis; eczema; ulcerative colitis;

glomerular nephritis; scleroderma; chronic thyroiditis; Grave's disease; Ormond's disease; autoimmune gastritis; myasthenia gravis; autoimmune hemolytic anemia; autoimmune neutropenia; thrombocytopenia; pancreatic fibrosis; chronic active hepatitis including hepatic fibrosis; acute and chronic renal disease; renal fibrosis; diabetic nephropathy; irritable bowel syndrome; pyresis; restenosis; cerebral malaria; stroke and ischemic injury; neural trauma; Alzheimer's disease; Huntington's disease; Parkinson's disease; acute and chronic pain;

allergies, including allergic rhinitis and allergic conjunctivitis; cardiac hypertrophy, chronic heart failure; acute coronary syndrome; cachexia; malaria; leprosy; leishmaniasis; Lyme disease; Reiter's syndrome; acute synoviitis; muscle degeneration, bursitis; tendonitis;

tenosynoviitis; herniated, ruptured, or prolapsed intervertebral disk syndrome; osteopetrosis; thrombosis; silicosis; pulmonary sarcosis; bone resorption diseases, such as osteoporosis or multiple myeloma-related bone disorders; cancer, including but not limited to metastatic breast carcinoma, colorectal carcinoma, malignant melanoma, gastric cancer, and non-small cell lung cancer; graft-versus-host reaction; and auto-immune diseases, such as multiple sclerosis, lupus and fibromyalgia; AIDS and other viral diseases such as Herpes Zoster, Heipes Simplex 1 or II, influenza virus, Severe Acute Respiratory Syndrome ( SARS) and cytomegalovirus: and diabetes mellitus. In addition, the methods of the embodiments can be used to treat proli erative disorders (including both benign and malignant hyperplasias), including ac me myelogenous leukemia, chronic myelogenous leukemia, Kaposi's sarcoma, metastatic melanoma, multiple myeloma, breast cancer, including metastatic breast carcinoma; colorectal, carcinoma; malignant melanoma; gastric cancer; non-small cell lung cancer (NSCfC): bone metastases, and the l ike; pain disorders including neuromuscular pain, headache, cancer pain, dental pain, and arthritis pain; angiogenic disorders including solid tumor angiogenesis. ocular neovascularization, and infantile hemangioma; conditions associated with the cyclooxygenase and lipoxygenase signaling pathways, including conditions associated with prostaglandin endoperoxide synthase- 2 (including edema, fever, analgesia, and pain); organ hypoxia; thrombin-induced platelet aggregation; protozoal diseases.

[0028] As used herein, a patient in need of "fiuvoxamine therapy" is understood to be a patient in need of "selective serotonin reuptake inhibitor (SSRI) therapy." Such patients include patients suffering from social anxiety disorder (social phobia), obsessive compulsive disorder (OCD), depression, anxiety disorders, panic disorder and post-traumatic stress disorder.

[0029] For CYP enzymes, the FDA generally defines a "strong inhibitor" as one that caused a > 5-fold increase in the plasma AUC values or more than 80% decrease in clearance of CYP substrates (not limited to sensitive CYP substrate) in clinical evaluations. The FDA generally defines a "moderate inhibitor" as one that caused a > 2- but < 5-fold increase in the AUC values or 50-80% decrease in clearance of sensitive CYP substrates when the inhibitor was given at the highest approved dose and the shortest dosing interval in clinical evaluations.

CYP inhibitors and substrates

[0030] In any of the embodiments described herein, including but not limited to providing pirfenidone for use in treating a patient, the use of pirfenidone in the manufacture of a medicament for treating a patient in need of pirfenidone therapy, and treatment methods involving the advice, warnings, discontinuation or dose titration downwards, the packages and kits, and/or the methods of preparing or packaging pirfenidone, the pirfenidone, uses, methods, packages, kits, advice, warnings, discontinuation or dose titration may apply not only to fiuvoxamine but also to any other drug that is a moderate to strong inhibitor of both CYP1A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, and/or CYP2C19 (or a drug that is a strong inhibitor of CYP1A2 that also has inhibitory effects on other CYP isozymes [2C9, 2C 19, and/or 3A4]), such as fiuvoxamine. The embodiments may also apply to any other drug that is a moderate to strong inhibitor of both CYP1A2 and another CYP enzyme selected from the group consisting of CYP3A4. CYP2C9, CYP2C1 9, CYP2B6, and/or CYP2D6. The embodiments may also apply to any other drug that is a moderate to strong inhibitor of both ( ΎΡ 1 A2 and another CYP enzyme that metabolizes pirfenidone, e.g. selected from the group consisting of CYP 1 A l , CYP2A6, W

CYP2B6, CYP2C8, CYP2C9, CYP2C18, CYP2C19, CYP2D6, CYP2E1 , CYP2J2 CYP3A4, CYP3A5, CYP4A 1 1 and/or CYP4F2.

[0031 J As yet other alternatives, in any of the embodiments described herein, including but not limited to the pirfenidone for use in treating a patient, the use of pirfenidone in the manufacture of a medicament for treating a patient in need of pirfenidone therapy, and treatment methods involving the advice, warnings, discontinuation or dose titration downwards, the packages and kits, and/or the methods of preparing or packaging pirfenidone, the pirfenidone, uses, methods, packages, kits, advice, warnings, discontinuation or dose titration may apply not only to fluvoxamine but also to any other drug that is a strong inhibitor of CYP1 A2 or a substrate for CYP1A2.

[0032] CYP1 A2 metabolizes many commonly used drugs including theophylline, imipramine, propranolol, and clozapine. These drugs are commonly referred to as

"substrates" for CYP1 A2. Additional CYP1A2 substrates include but are not limited to acetaminophen, amitriptyline, caffeine, chlordiazepoxide, einacalcet, clomipramine, clopidogrel, cyclobenzaprine, desipramine, diazepam, duloxetine, erlotinib, estradiol, fiutamide, halopendol, levobupivacame, methadone, mirtazapine, naproxen, nortriptyline, olanzapine, ondansetron, ramelteon, riluzole, ropinirole, ropivacaine, tacrine, tizamdine, verapamil, and warfarin.

[0033 | Inhibitors of CYP1 A2 include fluvoxamine, cimetidine, amiodarone, echinacea, enoxacin, norfloxacin, oral contraceptives, tacrine, ticlopidine, and many fluoroquinolone antibiotics. Moderate inhibitors of CYP1A2 include ciprofloxacin, mexiletine, propafenone and zileuton. Additional inhibitors of CYP1 A2 include atazanavir, citalopram,

clarithromycin, dilitiazem, erythromycin, ethinyl estradiol, isoniazid, ketoconazole, methoxsalen, nalidixic acid, norethindrone, omeprazole, paroxetine, tipranavir, and troleandomycin. Other inhibitors of CYP1A2 include acyclovir, caffeine, famotidine, fiutamide, grape ruit juice, lidocaine, lomeftoxacin, moclobemide, ofloxacin, perphenazine, phenacetin, propafenone, ropinirole, tocainide, and verapamil.

[0034] Inhibitors of CYP3A4 include amiodarone, cimetidine, ciprofloxacin, delavirdine, fluvoxamine, miconazole, and voriconazole (VFFN'D). Strong inhibitors of CYP3A4 include atazanavir, clarithromycin, indinavir, itraconazole, ketoconazole, nefazodone, nelfinavir, ritonavir, saquinavir and telithromycin. Moderate inhibitors of CYP3A4 include amprenavir, aprepitant, diltiazem, erythromycin, fluconazole, fosamprenavir, grapefruit juice and verapamil. Additional inhibitors of CYP3A4 i nclude acitretin, cyclosporine, danazol, diethyldithiocarbamate, efavirenz, ethinyl estradiol, fl uoxetine, gestodene, imatinib, isoniazid, metronidazole, methylpredisolone, mifepristone, nicardipine, nifedipine, norethindrone, norfloxacin, norfhioxetine, oxiconazole, pomegranate, prednisone, quinine, ranolazine, roxithromycin, sertraline, Synercid, troleandomycin, zafirlukast, and zileuton. Other inhibitors of CYP3A4 include doxycycline, echinacea, and enoxacin.

[0035] Inhibitors of CYP2C9 include cimetidine, delavirdine, efavirenz, fenofibrate (Tricor), fluoxetine, fluvastatin, fluvoxamine, isoniazid, ketoconazole, leflunomide, modafmil, sertraline, voriconazole (VFEND), and zafirlukast (Accolate). Moderate inhibitors of CYP2C9 include amiodarone, fluconazole and oxandrolone. Additional CYP2C9 inhibitors include atazanavir, chloramphenicol, clopidogrel, cotrimoxazole, cranberry, disulfiram, fluorouracil, gemfibrozil, ginkgo, imatinib, itraconazole, lovastatin,

metronidazole, omeprazole, paroxetine, sulfonamides, triclopidine, and tipranavir. Other inhibitors of CYP2C9 include anastrazole, phenylbutazone, sulfamethoxazole,

sulfaphenazole, tamoxifen, teniposide, valproic acid, and 5-fluorouracil.

[0036J Inhibitors of CYP2D6 include amiodarone, bupropion, celecoxib,

chlorpheniramine, cimetidine, cinacalcet, citalopram, clomipramine, desipramine, diphenhydramine, halofantrine, haloperidol, methadone, moclobemide, propafenone, ritonavir, sertraline, and thioridazine. Strong CYP2D6 inhibitors include fluoxetine, paroxetine and quinidine, while moderate CYP2D6 inhibitors include duloxetine and terbinafine. Additional inhibitors of CYP2D6 include chloroquine, cocaine, darifenacin, escitalopram, fluphenazine, hydroxychloroquine, imatinib, levomepromazine, norfhioxetine, perphenazine, pomegranate, propoxyphene, propranolol, quinacrine, ranitidine, ranolazine, and tipranavir. Other inhibitors of CYP2D6 include amitriptyline, chlorpromazine, doxepm, fluvoxamine, goldenseal, hydroxyzine, imipramine, metoclopramide, pimozide, and ticlopidine (Ticlid).

[0037J Inhibitors of CYP2C 19 include delavirdine, efavirenz, esomeprazole, felbamate, fluconazole, fluoxetine, fluvoxamine, indomethacin, isoniazid (INH), modafmi l ( Provigil), oxcarbazepine, ticlopidine, topiramate, and voriconazole (VFEND) A strong inh ibitor of CYP2C19 is omeprazole. Additional inhibitors of CYP2C 19 include citalopram, fluvastatin, ketoconazole, lansoprazole, letrozole, paroxetine, sertraline, telmisartan, and tipranavi r.

Other inhibitors of CYP2C19 include artemisini n. chloramphenicol, and oral contraceptives. [0038J Inhibitors of CYP2B6 include clopidogrel (Plavix), efavirenz, fluoxetine, fluvoxamine, ketoconazole, memantine, nelfinavir, oral contraceptives, paroxetine, ritonavir, thiotepa, and ticlopidine (Ticlid).

Avoiding or discontinuing administration of a drug to avoid adverse drug interactions with pirfenidone

[0039] As used herein, the term "avoid" and forms thereof are contemplated to have as alternatives the terms abstain, desist, forbear, and refrain, and forms thereof. In some cases, the alternative terms will be equivalent. For example, "avoiding" means "refraining from." Merriam- Webster Online Dictionary, 1 1 ^th ed., 24 November 2009. As used herein, the term "discontinue" and forms thereof are contemplated to have as alternatives the terms cease, stop, suspend, and quit. In the methods described herein, the avoiding and/or discontinuing steps can be performed in anticipation of pirfenidone therapy. For example, impending or imminent pirfenidone administration can be the proximate cause of the avoiding and/or discontinuing steps. As another example, concurrent pirfenidone administration can be the proximate cause of discontinuing and/or further avoiding steps.

|0040] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy (e.g. , a patient with IPF), involving administering to the patient a therapeutically effective amount of pirfenidone, and avoiding or contraindicating administration of a CYP 1 A2 inhibitor. In some embodiments, the CYP1A2 inhibitor is a strong CYP1A2 inhibitor. In some embodiments, the CYP1A2 inhibitor is a moderate to strong CYP1 A2 inhibitor. In some embodiments, the CYP1 A2 inhibitor is a drug that is a moderate-strong inhibitor of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 19 and/or CYP3A4 (or a drug that is a strong inhibitor of CYP1 A2 that also has inhibitory effects on other CYP isozymes [2C9, 2C 19, and/or 3A4]), or a drug that is a moderate to strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C 19, CYP2B6, and/or CYP2D6. In some embodiments, the drug is fluvoxamine.

[0041] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy (e.g. , a patient with IPF), involving administering to the patient a therapeutically effective amount of pirfenidone, and avoiding or contraindicating administration of a moderate-strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of C^' YP IAI , CYP2A6, CYP2B6, CY P2C8, CYP2C9, CYP2C 1 8, CYP2C 19, CYP2D6, CYP2E 1 , CYP2J2 CYP3A4, CYP3A5,

CYP4A1 1 and/or CYP4F2.

(0042] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy (e.g. , a patient with IPF), involving administering to the patient a therapeutically effective amount of pirfenidone, and avoiding or contraindi eating administration of a strong CYP1 A2 inhibitor.

[0043] lⁿ some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy (e.g. , a patient with IPF), involving administering to the patient a therapeutically effective amount of pirfenidone, and avoiding or contraindicating administration of a CYP l A2 substrate.

[0044] In other aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy, comprising discontinuing administration of a drug that is a moderate-strong inhibitor of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and/or CYP3A4 (or a drug that is a strong inhibitor of CYPl A2 that also has inhibitory effects on other CYP isozymes [2C9, 2C19, and/or 3A4]) to avoid an adverse drug interaction, and administering a therapeutically effective amount of pirfenidone. In some embodiments, the dmg being discontinued is a drug that is a moderate to strong inhibitor of both CYP l A2 and another CYP enzyme selected from the group consisting o f CYP3A4, CYP2C9, CYP2C 19, CYP2B6, and/or CYP2D6. In some embodiments, the drug is fluvoxamine.

[0045| In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy, comprising discontinuing administration of a drug that is a moderate-strong inhibitor of both CYP l A2 and another CYP enzyme selected from the group consisting of CYP 1 A1 , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C 1 8, CYP2C 19, CYP2D6, CYP2E 1 , CYP2J2 CYP3A4, CYP3A5, CYP4A 1 I and/or CYP4F2 to avoid an adverse drug interaction, and adm i nistering a therapeutically e ffective amount of pirfenidone.

[0046] In other aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy, comprising discontinuing administration of a drug that is a strong CYP1A2 inhibitor to avoid an adverse drug interaction, and administering a therapeutically effective amount o f pirf enidone. In other aspects, the invention provides a method of administering pri fenidone therapy to a patient in need of pirfenidone therapy, comprising discontinuing administration of a drug that is a CYP l A2 inhibitor, e.g. a moderate to strong CYP1A2 inhibitor.

[0047] In one example, in a method of administering a therapeutically effective amount of pirfenidone to a patient with IPF, the invention provides an improvement that comprises avoiding, contraindicatmg or discontinuing administration of the drug that is a CYP inhibitor and administering a therapeutically effective amount of pirfenidone.

[0048] In some embodiments, the drug that is a CYP inhibitor is discontinued concurrent with starting administration of pirfenidone. In other embodiments, the drug that is a CYP inhibitor is discontinued within at least 3 days to 1 month prior to or after starting pirfemdone therapy. This time period, for example, permits adequate time for tapering and withdrawal without adverse effects.

[0049] Thus, an aspect of the invention provides pirfenidone for use in treating a patient in need of pirfenidone therapy, characterized in that the treating comprises avoiding, contraindicating or discontinuing concomitant use (or co-administration) of a strong CYPl A2 inhibitor; or a moderate to strong CYPl A2 inhibitor; or a drug that is a moderate-strong inhibitor of both CYPl A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and/or CYP3A4; or a drug that is a strong inhibitor of C YPl A2 that also has inhibitory effects on other CYP isozymes [2C9, 2C 19, and/or 3A4]; or a drug that is a moderate-strong inhibitor of both CYPl A2 and another CYP enzyme selected from the group consisting of CYPl Al , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C18, CYP2C 19, CYP2D6, CYP2E 1 , CYP2.I2 CYP3A4, CYP3A5, CYP4A 1 1 and/or CYP4F2; or fluvoxamine (collectively referred to as "CYPl A2 inhibitors"). In some embodiments, the concomitant use of the CYPl A2 inhibitor is avoided, contraindicated or discontinued, in order to avoid reduced clearance of pirfenidone, or the potential for reduced clearance of pirfenidone. In some embodiments, the concomitant use of the CYP l A2 inhibitor is avoided, contraindicated or discontinued, in order to avoid increased exposure to pirfenidone, or the potential for increased exposure to pirfenidone. Administration of pirfenidone in patients that

concomitantly use or are being administered fluvoxamine results in about a 6-fold increase in pirfenidone exposure. Il is understood that any of the aspects or embodiments or examples described herein with respect to methods of treatment apply to this aspect of the invention that provides pirfenidone for use in treating a patient For example, the patient may be a patient with IPF, and the therapeutically effective amount administered may be 2400 or 2403 mg per day. [0050] Similarly, a further aspect of the invention provides the use of pirfenidone in the manufacture of a medicament for treating a patient in need of pirfenidone therapy, characterized in that the treating comprises avoiding, contraindicating or discontinuing concomitant use (or co-administration) of a CYPl A2 inhibitor. It is understood that any of the aspects or embodiments or examples described herein with respect to methods of treatment or "pirfenidone for use" in treating a patient apply to this aspect of the invention that provides for the use of pirfenidone in manufacture of a medicament. For example, the patient may be a patient with IPF, and the therapeutically effective amount administered may be 2400 or 2403 mg per day.

[0051 ] In some embodiments, the patient is a patient in need of therapy with a CYPl A2 inhibitor. In some embodiments, the patient is a patient in need of therapy with a strong CYPl A2 inhibitor. In some embodiments, the patient is a patient in need of therapy with a moderate to strong CYP 1 A2 inhibitor. In some embodiments, the patient is a patient in need of therapy with a drug that is a moderate-strong inhibitor of both CYP l A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and/or CYP3A4; or a drug that is a strong inhibitor of CYPl A2 that also has inhibitory effects on other CYP isozymes [2C9, 2C19, and/or 3A4]. In some embodiments, the patient is a patient in need of fluvoxamine therapy. In some embodiments, the patient is a patient who is avoiding concomitant use of the CYPl A2 inhibitor, e.g. because concomitant use of pirfenidone with the CYPl A2 inhibitor is contraindicated or to be used with caution. In some embodiments, the patient is a patient who was or is being administered the CYPl A2 inhibitor. In some embodiments, the patient is a patient who is discontinuing use of the CYPl A2 inhibitor prior to the initiation of pirfenidone therapy in order to avoid reduced clearance (or increased exposure to) pirfenidone, or the potential for reduced c learance of (or increased exposure to) pirfenidone. In some embodiments, the patient is a patient who is discontinuing

administration of the the CYPl A2 inhibitor, within 1 month, or within 2 weeks, prior to starting pirfenidone therapy, or concurrent with starting pirfenidone therapy. It is understood that any of the aspects or embodiments or examples described herein with respect to methods of treatment apply to this aspect of the invention that provides for characterization of the patients to be treated with pirfenidone.

[0052] In some embodiments, the concomitant use f the CYP l A2 inhibitor is avoided, contraindicated or discontinued in order to:

(a) avoid altering the therapeutic effect profi le of pirfenidone, and/or (b) avoid altering the adverse reaction profile of pirfenidone, and/or

(c) avoid the increased exposure or potential for increased exposure, and/or

(d) avoid the reduced clearance or potential for reduced clearance, and/or

(e) avoid the average 6-fold increase in exposure to pirfenidone upon concomitant administration with fluvoxamine, and/or

(f) avoid the average 2-fold increase in average peak serum concentration of pirfenidone (Cmax) upon concomitant administration with fluvoxamine, and/or

(g) reduce toxicity of pirfenidone treatment, and/or

(h) improve safety of pirfenidone treatment, and/or

(i) reduce adverse drug interaction associated with pirfemdone treatment.

[0053] In some embodiments in which fluvoxamine is discontinued to avoid an adverse drug interaction, fluvoxamine is discontinued within at least 3 days prior to or after starting pirfenidone therapy. In various embodiments, fluvoxamine is discontinued within at least 4 days, or at least 5 days, or at least 6 days, or at least 7 days (or one week), or at least 8 days, or at least 9 days, or at least 10 days, or at least 1 1 days, or at least 12 days, or at least 13 days, or at least 14 days (or two weeks), or at least 15 days, or at least 16 days, or at least 17 days, or at least 18 days, or at least 19 days, or at least 20 days, or at least 21 days (or three weeks), or at least 22 days, or at least 23 days, or at least 24 days, or at least 25 days, or at least 26 days, or at least 27 days, or at least 28 days (or four weeks), or at least 29 days, or at least 30 days, or at least one month, prior to or after starting pirfenidone therapy. In some embodiments, the fluvoxamine is discontinued no earlier than one month, 3 weeks, 2 weeks or 1 week before starting pirfenidone therapy. Preferably, sufficient time is allowed for tapering and/or withdrawal of fluvoxamine therapy.

[0054] In some embodiments in which the drug being discontinued is a CYP inhibitor, the drug is discontinued within at least 3 days prior to or after starting pirfenidone therapy. In various embodiments, the drug that is a CYP inhibitor is discontinued within at least 4 days, or at least 5 days, or at least 6 days, or at least 7 days (or one week), or at least 8 days, or at least 9 days, or at least 1 0 days, or at least 1 1 days, or at least 12 days, or at least 1 3 days, or at least 14 days (or two weeks), or at least 15 days, or at least 16 days, or at least 1 7 days, or at least 18 days, or at least 19 days, or at least 20 days, or at least 21 days (or three weeks), or at least 22 days, or at least 23 days, or at least 24 days, or at least 25 days, or at least 26 clays, or at least 27 days, or at least 28 days (or four weeks), or at least 29 days, or at least 30 davs, or at least one month, prior to or after starting pirfenidone therapy. In some embodiments, the drug that is a CYP inhibitor is discontinued no earlier than one month, 3 weeks, 2 weeks or 1 week before starting pirfenidone therapy. Preferably, sufficient time is allowed for tapering and/or withdrawal of the drug upon discontinuation.

[0055] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy, comprising discontinuing administration of the CY 1 A2 substrate to avoid an adverse drug interaction and administering a therapeutically effective amount of pirfenidone. In some embodiments, the drug that is a CYP1A2 substrate is discontinued concurrent with starting administration of pirfenidone. In other embodiments, the drug that is a CYP1A2 substrate is discontinued within at least 3 days to 1 month prior to or after starting pirfenidone therapy. This time period, for example, permits adequate time for tapering and withdrawal without adverse effects.

[0056] In some embodiments in which a CYP1 A2 substrate is discontinued to avoid an adverse drug interaction, the CYP1A2 substrate is discontinued within at least 3 days prior to or after starting pirfenidone therapy. In various embodiments, the CYP1A2 substrate is discontinued within at least 4 days, or at least 5 days, or at least 6 days, or at least 7 days (or one week), or at least 8 days, or at least 9 days, or at least 10 days, or at least 1 1 days, or at least 12 days, or at least 13 days, or at least 14 days (or two weeks), or at least 15 days, or at least 16 days, or at least 1 7 days, or at least 1 8 days, or at least 19 days, or at least 20 days, or at least 21 days (or three weeks), or at least 22 days, or at least 23 days, or at least 24 days, or at least 25 days, or at least 26 days, or at least 27 days, or at least 28 days (or four weeks), or at least 29 days, or at least 30 days, or at least one month, prior to or after starting pirfenidone therapy. In some embodiments, the CYP1A2 substrate is discontinued no earlier than one month, 3 weeks, 2 weeks or 1 week before starting pirfenidone therapy. Preferably, sufficient time is allowed for tapering and/or withdrawal of the CYP 1 A2 substrate therapy.

Selecting an alternative drug to administer concurrently with pirfenidone therapy

[0057] In some aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy and in need of therapy with a drug that is a moderate-strong inhibitor of both CYP1A2 and another CYP enzyme selected from the group consisting of CYP1 A 1 , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C18, CYP2C 1 9.

CYP2D6, CYP2E1 , CYP2J 2 CYP3A4, CYP3A5, CYP4A 1 1 and/or CYP4F2, comprising administering a therapeuiieally effective amount of pirfenidone to the patient, and

administering an alternative therapy that is not a moderate-strong inhibitor of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP1A1 , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C 18, CYP2C 19, CYP2D6, CYP2E1 , CYP2J2 CYP3A4, CYP3A5, CYP4A 1 1 and/or CYP4F2.

[0058] In another embodiment, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy and in need of therapy with a drug that is a moderate-strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19, CYP3A4, CYP2B6 and/or CYP2D6, comprising administering a therapeutically effective amount of pirfenidone to the patient, and administering an alternative therapy that is not a moderate-strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19, CYP3A4, CYP2B6 and/or CYP2D6.

[0059] In some embodiments, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy and in need of therapy with a drug that is a moderate-strong inhibitor of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19, and/or CYP3A4, comprising administering a therapeutically effective amount of pirfenidone to the patient, and administering an alternative therapy that is not a moderate-strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 19, and/or CYP3A4.

[0060] In other aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy and in need of therapy with a drug that is a strong CYP1 A2 inhibitor, comprising administering a therapeutically effective amount of pirfenidone to the patient, and administering an alternative therapy that is not a strong CYP1A2 inhibitor.

[0061] In yet other aspects, the invention provides a method of administering pirfenidone therapy to a patient in need of pirfenidone therapy and in need of therapy with a drug that is a CYP1A2 substrate, comprising administering a therapeutically effective amount of pirfenidone to the patient, and administering an alternative therapy that is not a CYP 1 A2 substrate.

Improving administration of pirfenidone by advising or cautioning patient

[0062] The administration of a therapeutically effective amount of pirfenidone to a patient in need of pirfenidone therapy can be improved. In some embodiments, the patient is advised that co-administration of pirfenidone with drugs that are a mo derate- strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 1 and/or CYP3A4 can alter the therapeutic effect or adverse reaction profile of pirfenidone. In some embodiments, the patient is advised that co-administration of pirfenidone with fluvoxamine can alter the therapeutic effect or adverse reaction profile of pirfenidone. In some embodiments, the patient is advised that co-administration of pirfenidone with drugs that are a moderate-strong inhibitor of both CYPl A2 and another CYP enzyme selected from the group consisting of CYP l A l , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C 18, CYP2C 19, CYP2D6, CYP2E1 , CYP2J2 CYP3A4, CYP3A5,

CYP4A 1 1 and/or CYP4F2, can alter the therapeutic effect or adverse reaction profile of pirfenidone. In some embodiments, the patient is advised that co-administration of pirfenidone with a drug that is a strong CYP1A2 inhibitor can alter the therapeutic effect or adverse reaction profile of pirfenidone. In some embodiments, the patient is advised that coadministration of pirfenidone with a drug that is a CYP l A2 substrate can alter the therapeutic effect or adverse reaction profile of pirfenidone.

[0063] In some embodiments, the patient is advised that use of pirfenidone in patients being treated with fluvoxamine is contraindicated. In some embodiments, the patient is advised that co-administration of pirfenidone and fluvoxamine resulted in a 6-fold increase in exposure to pirfenidone.

[0064] In some embodiments, the patient is advised that use of pirfenidone in patients being treated with a drug that is a moderate-strong inhibitor of both CYPl A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and/or CYP3A4 is contraindicated. In some embodiments, the patient is advised that pirfenidone should be used with caution in patients taking a drug that is a moderate-strong inhibitor of both CYPl A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and/or CYP3A4.

[0065] In some embodiments, the patient is advised that use of pirfenidone in patients being treated with a drug that is a moderate-strong inhibitor of both CYP1A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 19, CYP3A4, CYP2B6 and/or CYP2D6 is contraindicated. In some embodiments, the patient is advised that pirfenidone should be used with caution in patients taking a drug that is a moderate-strong inhibitor of both CYPl A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19, CYP3A4, CYP2B6 and/or CYP2D6.

Dosing and dose modifications (0066] In various embodiments, a method of administering pirfenidone and fiuvoxamine concurrently is provided wherein the patient is administered a therapeutically effective amount of fiuvoxamine and a dosage of pirfenidone that is decreased relative to a patient not taking fiuvoxamine. In some aspects, such a decreased dosage of pirfenidone is less than 2400 mg/day. For example, the decreased dosage is about 2136 mg per day, 1869 mg per day, 1602 mg per day, 1335 mg per day, or 1068 mg per day (e.g., 8, 7, 6, 5, 4, or 3 capsules per day where each capsule is approximately 267 mg). In some embodiments, the patient is already being administered fiuvoxamine. In other embodiments, the patient is already being administered pirfenidone. In related embodiments, the dosage of pirfenidone is decreased prior to administration of fiuvoxamine.

[0067] In other aspects, a method of administering pirfenidone and a drug that is a moderate-strong inhibitor of both CYP1A2 and another CYP enzyme selected from the group consisting of CYP1A1 , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C 18, CYP2C19, CYP2D6, CYP2E1, CYP2J2 CYP3A4, CYP3A5, CYP4A1 1 and/or CYP4F2 concurrently is provided wherein the patient is administered a therapeutically effective amount of the drug that is a CYP inhibitor and a dosage of pirfenidone that is decreased relative to a patient not taking such drug that is a CYP inhibitor. In some aspects, such a decreased dosage of pirfenidone is less than 2400 mg/day. For example, the decreased dosage is about 2136 mg per day, 1869 mg per day, 1602 mg per day, 1335 mg per day, or 1068 mg per day (e.g., 8, 7, 6, 5, 4, or 3 capsules per day where each capsule is approximately 267 mg). In some embodiments, the patient is already being administered the drug that is a CYP inhibitor. In other embodiments, the patient is already being administered pirfenidone. In related embodiments, the dosage of pirfenidone is decreased prior to administration of the drug that is a CYP inhibitor.

[0068] In other aspects, a method of administering pirfenidone and a drug that is a moderate-strong inhibitor of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 1 and/or CYP3A4 concurrently is provided, wherein the patient is administered a therapeutically effective amount of the drug that is a CYP inhibitor and a dosage of pirfenidone that is decreased relative to a patient not taking such drug that is a CYP inhibitor. In related aspects, a method of administeri ng pirfenidone and a drug that is a moderate-strong inhibitor of both CYP1A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19, CYP3A4, CYP2BO and/or CYP2D6 concurrently is provided, wherein the patient is administered a therapeutical !} e ffective amount of the drug that is a CYP inhibitor and a dosage of pirfenidone that is decreased relative to a patient not taking such drug that is a CYP inhibitor. In some aspects, such a decreased dosage of pirfenidone is less than 2400 mg/day. For example, the decreased dosage is about 2136 mg per day, 1869 mg per day, 1602 mg per day, 1335 mg per day, or 1068 mg per day (e.g. , 8, 7, 6, 5, 4, or 3 capsules per day where each capsule is approximately 267 mg). In some embodiments, the patient is already being administered the drag that is a CYP inhibitor. In other embodiments, the patient is already being administered pirfenidone. In related embodiments, the dosage of pirfenidone is decreased prior to administration of the drug that i a CYP inhibitor.

[0069] In yet other aspects, a method of administering pirfenidone and a strong CYPl A2 inhibitor concurrently is provided wherein the patient is administered a therapeutically effective amount of the strong CYP1A2 inhibitor and a dosage of pirfenidone that is decreased relative to a patient not taking the strong CYPl A2 inhibitor. In some aspects, such a decreased dosage of pirfenidone is less than 2400 mg/day. For example, the decreased dosage is about 2136 mg per day, 1869 mg per day, 1602 mg per day, 1335 mg per day, or 1068 mg per day (e.g. , 8, 7, 6, 5, 4, or 3 capsules per day where each capsule is

approximately 267 mg). In some embodiments, the patient is already being administered the strong CYPl A2 inhibitor. In other embodiments, the patient is already being administered pirfenidone. In related embodiments, the dosage of pirfenidone is decreased prior to administration of the strong CYP 1 A2 inhibitor.

|0070] In various embodiments, a method of administering pirfenidone and a CYPl A2 substrate concurrently is provided wherein the patient is administered a therapeutically effective amount of the CYP l A2 substrate and a dosage of pirfenidone that is decreased relative to a patient not taking the CYP l A2 substrate. In some aspects, such a decreased dosage of pirfenidone is less than 2400 mg/day. For example, the decreased dosage is about 2136 mg per day, 1869 mg per day. 1602 mg per day, 1335 mg per day, or 1068 mg per day (e.g. , 8, 7, 6, 5, 4, or 3 capsules per day where each capsule is approximately 267 mg). In some embodiments, the patient is already being administered the CYPl A2 substrate. In other embodiments, the patient is already being administered pirfenidone. In related embodiments, the dosage of pirfenidone is decreased prior to administration of the CYP1A2 substrate.

[0071 J In some embodiments, the amount of pirfenidone being administered is 2400 or 2403 mg day. Pirfenidone can be dosed at a total amount of about 50 to about 2400 mg per lay. The dosage can be divided into two or three doses over the day or given in a single dailv dose. Specific amounts of the total daily amount of the therapeutic contemplated for the disclosed methods include about 50 mg, about 100 mg, about 1 5< > mg, about 200 mg, about 250 mg, about 267 mg, about 300 mg, about 350 mg, about 400 mg, about 450 mg, about 500 mg, about 534 mg, about 550 mg, about 600 mg, about 650 mg, about 700 mg, about 750 mg, about 800 mg, about 850 mg. about 900 mg, about 950 mg, about 1000 mg, about 1050 mg, about 1068 mg, about 1 100 mg, about 1 150 mg, about 1200 mg, about 1250 mg, about 1300 mg, about 1335 mg, about 1350 mg, about 1400 mg, about 1450 mg, about 1500 mg, about 1550 mg, about 1600 mg, about 1650 mg, about 1700 mg, about 1 750 mg, about 1800 mg, about 1 850 mg, about 1869 mg, about 1900 mg, about 1950 mg, about 2000 mg, about 2050 mg, about 2100 mg, about 21 36 mg, about 2150 mg, about 2200 mg, about 2250 mg, about 2300 mg, about 2350 mg, and about 2400 mg.

[0072] Dosages of pirfenidone can alternately be administered as a dose measured in mg/kg. Contemplated mg/kg doses of the disclosed therapeutics include about 1 mg/kg to about 40 mg kg. Specific ranges of doses in mg/kg include about 1 mg/kg to about 20 mg/kg, about 5 mg/kg to about 20 mg/kg, about 10 mg/kg to about 20 mg/kg, about 10 mg/kg to about 30 mg/kg, and about 15 mg/kg to about 25 mg/kg.

[0073] in one embodiment, a dosage amount of pirfenidone is taken with food. In another embodiment, the patient is instructed to administer the dosage of pirfenidone with food.

|0074] In some embodiments, a method of administering a SSR1 to a patient in need thereof is provided, the improvement comprising discontinuing administration of

fluvoxamine, for example, concurrent with starting administration of pirfenidone, and optionally administering an SSRI that is not a moderate to strong inhibitor of both CYP 1 A2, and a CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and/or

CYP3A4.

[0075] In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage of pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein co-administration of fluvoxamine to the patient does not result in an increased exposure to pirfenidone. In some embodiments, the dose is reduced by about 100 mg/day. In other embodiments, the dose is reduced by about 1 0 mg/day, or about 200 mg/day. or about 250 mg/day, or about 267 mg/day, or about 300 mg/day, or about 350 mg/day, or about 400 mg/day, or about 450 mg day. or about 500 mg day, or about 550 mg/day, or about 600 mg/day, or about 650 mg/day, or about 700 mg^'day, or about 750 mg/day, or about 800 mg day (to a total dai ly dose of about 1600 mg day or 1602 mg/day), or about 850 mg/day, or about 900 mg, day, or about 950 mg/day, or about 1000 mg/day, or about 1050 mg/day, or about 1 100 mg clay, or about 1 150 mg/day, or about 1200 mg/day, or about 1250 mg/day, or about 1300 mg/day, or about 1350 mg/day, or about 1400 mg/day, or about 1450 mg/day, or about 1500 mg/day, or about 1600 mg/day (to a total daily dose of about 800 mg/day or 801 mg/day) or more.

[0076] In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage o pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein co-administration of a drug that is a moderate-strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP1A1 , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C18, CYP2C 19, CYP2D6, CYP2E 1 , CYP2J2 CYP3A4, CYP3A5, CYP4A1 1 and/or CYP4F2 to the patient does not result in an increased exposure to pirfenidone. In some embodiments, the dose is reduced by about 100 mg/day. In other embodiments, the dose is reduced by about 150 mg/day, or about 200 mg/day, or about 250 mg/day, or about 267 mg/day, or about 300 mg/day, or about 350 mg/day, or about 400 mg/day, or about 450 mg/day, or about 500 mg/day, or about 550 mg/day, or about 600 mg/day, or about 650 mg/day, or about 700 mg/day, or about 750 mg/day, or about 800 mg/day (to a total daily dose of about 1600 mg/day or 1602 mg/day, or about 850 mg/day, or about 900 mg/day, or about 950 mg/day, or about 1000 mg/day, or about 1050 mg/day, or about 1 100 mg/day, or about 1 150 mg/day, or about 1200 mg/day, or about 1250 mg/day, or about 1300 mg/day, or about 1350 mg/day, or about 1400 mg/day, or about 1450 mg/day, or about 1500 mg/day, or about 1600 mg/day (to a total daily dose of about 800 mg/day or 801 mg/day) or more.

[0077| In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage of pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein co-administration of a drug that is a moderate-strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 19 and/or CYP3A4 to the patient does not result in an increased exposure to pirfenidone. In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage o f pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein coadm inistration of a drug that is a moderate-strong inhibitor of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C 19, CYP3A4, CYP2B6 and. or CYP2D6 to the patient does not result in an increased exposure to pirfenidone. In some embodiments, the dose is reduced by about 100 mg/day. In other embodiments, the dose is reduced by about 150 mg, day, or about 200 mg/day, or about 250 mg/day, or about 267 mg/day, or about 300 mg/day. or about 350 mg/day, or aboul 400 mg/day, or about 450 mg/day, or about 500 mg/day, or about 550 mg day, or about 600 mg/day, or about 650 mg/day, or about 700 mg/day, or about 750 mg/day, or about 800 mg/day (to a total daily dose of about 1600 mg/day or 1602 mg/day), or about 850 mg/day, or about 900 mg/day, or about 950 mg/day, or about 1000 mg day, or about 1050 mg/day, or about 1 100 mg/day, or about 1 1 50 mg/day, or about 1200 mg/day, or about 1250 mg/day, or about 1300 mg/day, or about 1350 mg/day, or about 1400 mg/day, or about 1450 mg/day, or about 1500 mg/day, or about 1600 mg/day (to a total daily dose of about 800 mg/day or 801 mg/day) or more.

[0078] In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage of pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein co-administration of a strong CYP 1 A2 inhibitor to the patient does not result in an increased exposure to pirfenidone. In some embodiments, the dose is reduced by about 100 mg/day. In other embodiments, the dose is reduced by about 150 mg/day, or about 200 mg/day, or about 250 mg/day, or about 267 mg/day, or about 300 mg/day, or about 350 mg/day, or about 400 mg/day, or about 450 mg/day, or about 500 mg/day, or about 550 mg/day, or about 600 mg/day, or about 650 mg/day, or about 700 mg/day, or about 750 mg/day, or about 800 mg/day (to a total daily dose of about 1600 mg/day or 1 602 mg/day), or about 850 mg/day, or about 900 mg/day, or about 950 mg/day, or about 1000 mg/day, or about 1050 mg/day, or about 1 100 mg/day, or about 1 150 mg/day, or about 1200 mg/day, or about 1250 mg/day, or about 1300 mg/day, or about 1350 mg/day, or about 1400 mg/day, or about 1450 mg/day, or about 1500 mg/day, or about 1600 mg/day (to a total daily dose of about 800 mg/day or 801 mg/day) or more.

[0079| In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage of pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein co-administration of a CYP 1A2 substrate to the patient does not result in an increased exposure to pirfenidone. In some embodiments, the dose is reduced by about 100 mg/day. In other embodiments, the dose is reduced by about 150 mg/day, or about 200 mg/day, or about 250 mg/day, or about 267 mg/day, or about 300 mg/day, or about 350 mg/day, or about 400 mg/day, or about 450 mg day, or about 500 mg/day, or about 550 mg/day, or about 600 mg/day, or about 650 mg/day, or about 700 mg/day, or about 750 mg/day, or about 800 mg/day (to a total daily dose of about 1600 mg/day or 1602 mg/day), or about 850 mg/day, or about 900 mg/day, or about 950 mg/day, or about 1000 mg. day, or about 1050 mg/day. or about 1 100 mg/day, or about 1 1 50 mg/day, or about 1200 mg day, or about 1250 mg/day. or about 1300 mg/day, or about 1350 mg/day, or about 1400 mg/day, or about 1450 mg/day, or about 1 500 mg/day, or about 1600 mg day (to a total daily dose of about 800 mg/day or 801 mg/day) or more.

[0080] In some embodiments, a method of administering pirfenidone therapy to a patient receiving fluvoxamine therapy is provided, comprising administering to the patient a therapeutically effective amount of fluvoxamine and administering to the patient a daily dosage of pirfenidone that is less than 2400 mg or 2403 mg per day, e.g. 1600 mg or 1602 mg per day. In some embodiments, the dosage of pirfenidone is decreased prior to administration of fluvoxamine. Similarly, in any of the foregoing embodiments relating to other CYP inhibitors or CYP substrates, the daily dosage of pirfenidone that is less than 2400 mg or 2403 mg per day may be, e.g. 1600 mg or 1602 mg per day.

[0081 ] In some embodiments, a method of optimizing pirfenidone therapy is provided comprising titrating the dosage of pirfenidone administered to a patient downward relative to a previously administered dosage in the patient, wherein co-administration of fluvoxamine to the patient does not result in an increased exposure to pirfenidone. It is understood that, in such embodiments comprising dose titration downwards, upon discontinuation of fluvoxamine, the dosage is titrated back up to a dose that is not less than 2400 or 2403 mg/day. As noted above, in any of the embodiments described herein, including but not limited to discontinuation or dose titration downwards, the packages and kits, and/or the methods of preparing or packaging pirfenidone, the pirfenidone, uses, methods, packages, kits, advice, warnings, discontinuation or dose titration may apply not only to fluvoxamine but also to (a) any other drug that is a moderate to strong inhibitor of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP3A4. CYP2C9, and/or CYP2C 19, or (b) a drug that is a strong inhibitor of CYPl A2 that also has inhibitory effects on other CYP isozymes [2C9, 2C 19, and/or 3A4]), or (c) any other drug that is a moderate to strong inhibitor of both CYP 1A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C 1 9, CYP2B6, and/or CYP2D6, or (d) any other drug that is a moderate to strong inhibitor of both CYPl A2 and another CYP enzyme that metabolizes pirfenidone, e.g. selected from the group consisting of CYPl Al , CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2C 18, CYP2C19, CYP2D6, CYP2E 1 , CYP2J2 CYP3A4, CYP3A5, CYP4A1 1 and/or ( ΎΡ4Ι \ or (e) any other drug that is a strong inhibitor of CYP l A2 or (i) any other drug that is a substrate for CYP 1A2.

Packages, kits, methods of packaging, and methods of delivering ( 0082J In another aspect, a package or kit is provided comprising pirfenidone, optionally in a container, and a package insert, package label, instructions or other labeling including any one, two, three or more of the following information or recommendations:

(a) use of fluvoxamine should be avoided or discontinued,

(b) co-administration of pirfenidone with drugs that are moderate to strong inhibitors of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, and/or CYP2C 19, can alter the therapeutic effect or adverse reaction profile of pirfenidone,

(c) co-administration of pirfenidone with fluvoxamine can alter the therapeutic effect or adverse reaction profile of pirfenidone,

(d) use of pirfenidone in patients being treated with fluvoxamine is contraindicated,

(e) co-administration of pirfenidone and fluvoxamine resulted in an average 6-fold increase in exposure to pirfenidone, and/or

(f) strong CYP 1 A2 inhibitors should be used with caution in patients receiving pirfenidone due to the potential for reduced pirfenidone clearance.

10083) In some embodiments, the information or recommendation may include that coadministration of pirfenidone and

resulted in a 2-fold increase in average peak serum concentration of pirfenidone (Cmax).

[00841 In other embodiments, the in formation or recommendation may include that coadministration of pirfenidone with drugs that are moderate to strong inhibitors of both CYP 1 A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C 1 , CYP2B6, and/or CYP2D6 can alter the therapeutic effect or adverse reaction profi le of pirfenidone. In other embodiments, the information or recommendation may include that co-administration of pirfenidone with drugs that are moderate to strong inhibitors of both (ΎΡ 1 A2 and another CYP enzyme selected from the group consisting of CYP 1A1 , CY P2A6. CYP2B6, CYP2C8, CYP2C9, C YP2C 18, CYP2C 19, CYP2 D6, CYP2E1 , CYP2J2 CYP A4. CYP3A5, CYP4A1 1 and/or CY P4F2 can alter the therapeutic effect or adverse reaction profile of pirfenidone. In other embodiments, the information or recommendation may incl ude that co-administration of pirfenidone with drugs that are strong CYP1A2 inhibitors can alter the therapeutic effect or adverse reaction profi le of pirfenidone. In other embodiments, the information or recom mendation may include that co-administration of W 201 pirfenidone with drugs that are CYP 1 A2 substrates can alter the therapeutic effect or adverse reaction profile of pirfenidone.

[0085] In other embodiments, the information or recommendation may include that drugs that are moderate to strong inhibitors of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, and/or CYP2C19 should be avoided or discontinued, or are contraindicated, or should be used with caution. In yet further embodiments, the information or recommendation may include that administering a strong CYP 1 A2 inhibitor should be avoided or discontinued, or are contraindicated, or should be used with caution. In other embodiments, the information or recommendation may include that drugs that are CY 1 A2 substrates should be avoided or discontinued, or are

contraindicated, or should be used with caution.

[0086] The package insert, package label, instructions or other labeling may further comprise directions for treating IPF by administering pirfenidone, e.g. , at a dosage of 2400 mg or 2403 mg per day.

[0087] In related aspect, the invention provides a method of preparing or packaging a pirfenidone medicament comprising packaging pirfenidone, optionally in a container, together with a package insert or package label or instructions including any one, two, three or more of the foregoing information or recommendations.

[0088] In some embodiments, a method of treating IPF is disclosed comprising providing, selling or delivering any of the kits of disclosed herein to a hospital, physician or patient.

[0089] In some embodiments, a kit is provided comprising fluvoxamine and a package insert, package label, instructions, or other labeling comprising any one, two, three or more of the follow ing warnings:

(a) use of fluvoxamine and pirfenidone is contraindicated

(b) use of pirfenidone in patients being treated with fluvoxamine is contraindicated, and/or

(c ) co-administration of pirfenidone and fluvoxamine resulted in an average 6-fold increase in exposure to pirfenidone.

(d ) co-administration of pirfenidone and fluvoxamine resulted in an average 2-fold increase i n peak semm concentration of pirfenidone. [0090] In some embodiments, a method of treating a patient in need of fluvoxamine is provided comprising providing or delivering any of the kits disclosed herein comprising fluvoxamine to a hospital, physician or patient.

[0091 ] In related aspects, the invention provides a method of administering a SSRI to a patient in need thereof, the improvement comprising discontinuing administration of fluvoxamine, for example, concurrent with starting administration of pirfenidone, and optionally administering an SSRI that is not a moderate to strong inhibitor of both CYP 1A2 and another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, and/or CYP2C19.

[0092| The invention will be more fully understood by reference to the following examples which detail exemplary embodiments of the invention. They should not, however, be construed as limiting the scope of the invention. All citations throughout the disclosure are hereby expressly incorporated by reference.

EXAMPLES

Example 1

[0093] An open-label Phase 1 study was performed to determine the impacts of fluvoxamine on the pharmacokinetics and safety of pirfenidone in healthy subjects.

[0094| Study Design. The study was a Phase 1 , open-label, parallel-group study in healthy subjects. Fifty-four subjects were to be enrolled in two groups, consisting of 27 subjects who were smokers (Group 1 ) and 27 subjects who were nonsmokers (Group 2). Smoking induces CYP 1A2 activity. Each group (smokers and nonsmokers) was to include a minimum of nine females and nine males, and attempts were to be made to enroll equal numbers of each sex in each group. Each subject was to receive a single 801 -mg dose of pirfenidone on Days 1 and 1 1 . Fluvoxamine dosing was started on Day 2 and titrated to the final dose according to the following schedule:

[0095| · Days 2 - 4: fluvoxamine 50 mg at bedtime

[0096] · Days 5 - 7: fluvoxamine 50 mg twice a day (in the morning and at bedtime)

[0097J ^♦ Days 8 - 1 1 : fluvoxamine 50 mg in the morning and 100 mg at bedtime

[0098| Al l pharmacokinetic (P ) anal ses were conducted using population PK methods using Monte-Carlo parametric expectation maximization as implemented in the open-source software program S ADAPT 1.5.6 (Bauer t /. , AAPS Journal 9( 1 ):E(>0-83, 2007). The structural model for the analysis was obtained from a preliminary population PK analysis. This population PK model was fit to the pirfenidone and 5 carboxy-pirfenidone plasma concentration-time data from Days 1 and 1 1 separately. Once a final population PK model was defined, AUCO- _Λ estimates were generated by simulating plasma PK profiles and compared for statistically significant differences between days (to test the effect of fl uvox amine co-administration) and between groups (to test the effect of smoking status).

[0099] As the primary endpoint of the study, differences in the pirfenidone and 5 carboxy pirfenidone AUCo-* estimates between Days 1 and 1 1 , and between smokers and nonsmokers were tested for significance. The analysis of the effect of fluvoxamine (i. e. , Day 1 versus Day 1 1 ) was analyzed using the FDA criteria for bioequivalence for paired data (FDA 2003). The ratio of AUCo-_∞ on Day 1 1 to that on Day 1 was used to test for the interaction between smoking status and fluvoxamine coadmi nistration. If other subject characteristics (such as body size or age) were also associated with the ratio of AUCo on Day 1 1 to that on Day 1 , the significance of these covariates was also tested. The significance of differences in pirfenidone and 5 -carboxy-pirfenidone AUCo__:» estimates on Day 1 in smokers and nonsmokers was tested using multivariable linear regression in order to take into account the effects of other significant covariates.

[0100] Ph armacokinetic Results. Fi fty-one of the 54 subjects enrolled in the study were included in the PK analyses. Three subjects were removed from the PK analyses as they did not meet the protocol-specified requirement for adequate compliance with the fluvoxamine dosing regimen. Two subjects discontinued the study early due to adverse events, and one subject only took 73% of the protocol-requi red fluvoxamine dose. All 5 1 subjects had the full complement of PK samples available for analysis. Each subject had two profiles on each day: one for pirfenidone and one for 5-carboxy pirfenidone. There were a total of 1224 samples ( 1 2 per subject per day); each sample was assayed for pirfenidone and 5-carboxy- pirfenidone for a total of 2448 concentrations.

[01011 A robust fit to the data was obtained using the population PK structural model. In general, the fits of the data were excellent: 98% of the individual profi les had r values above 0.9 and there was no systematic bias in the ti ts.

[0102] The summary statistics of AUC^'V , stratified by study day are provided in Table 1 . Symmetrical dot density plots of pirfenidone and 5-carboxy pirfenidone A UG)., values versus study day, identified by smoking status, are provided in Figure 1 . The coadministration o f fluvoxamine resulted i n a si gnificant increase in the At !(.^',>. , of pirfenidone (p < 0.00001). There was not a statistically significant effect of fluvoxamine coadministration on 5-carboxy pirtenidone AUCo-_^.

Table 1 Comparison of AUCQ._∞ Between Study Days (n=51 )

" p-value < O.OOO H i aired t-test)

u p-value = 0.168 (paired t-test)

AUCO-_Λ = area under the concentration-time curve from time zero to infinity; SD = standard deviation.

[0103] There was also a large apparent difference in the C_max estimates pre- and post- fluvoxamine; the pirfenidone C_max was higher after administration of fluvoxamine while the 5-carboxy pirfenidone Cmax was lower after administration of fluvoxamine. The mean (95%CI) for the ratio of C_max on Day 1 1 to the C_max on Day 1 was 2.09 ( 1.94 - 2.25) for pirfenidone and 0.369 (0.349 - 0.390) for 5-carboxy-pirfenidone.

[0104| The summary statistics of the ratio of the AUCo-/.. on Day 1 1 to the AUCo-/ on Day 1, stratified by smoking status, are provided in Table 2. While both smokers and nonsmokers were affected by the coadministration of fluvoxamine, smokers appeared to have a more pronounced increase in exposure to pirfenidone, as evidenced by the higher ratio of Day 1 1 to Day 1 AUC. Given that there was an imbalance in the demographics between smokers and nonsmokers (smokers were younger, heavier and predominantly male), the impact of these variables on the ratio of the pirfenidone AUCo-./. on Day 1 1 to the AUCo- /. on Day 1 was tested using multiple linear regression. Using backward elimination (p-value for

removal=0. 10), smoking status was the only signi ficant predictor of the ratio of the pirfenidone AUCo--r. on Day 1 1 to the AUCo- / on Day 1 ; body size, sex, and age were not significant.

Table 2 Comparison of Ratio of Day 11 AUC_0-∞ to Day 1 AUC_0-<» by

Smoking Status

Smoking Status Statistic Pirfenidone 5-Carboxy-Pirfenidone

AUCo-_∞ - area un er the concentrat on-t me curve rom time zero to nfin ty; SD = stan ar deviation.

[0105] In summary, the design and execution of this study allowed for a robust and informative analysis of the effects of CYP1 A2 inhibition on the pharmacokinetics of pirfenidone. Administration of the potent CYP inhibitor fluvoxamine resulted in a significant drag interaction and markedly increased pirfenidone exposure. Smokers were likely to experience significantly lower pirfenidone exposure (in the absence of the drug interaction) presumably due to the inductive effects of smoking.

[0106] The coadministration of fluvoxamine resulted in a significant drug interaction such that exposure (AUG). , ) to pirfenidone was, on average, nearly 6 times higher after ten days of dosing with fluvoxamine. Subjects also experienced, on average, a two-fold increase in Cmax after administration of fluvoxamine.

[0107] While the present invention has been described in terms of various embodiments and examples, it is understood that variations and improvements will occur to those skilled in the art.

Examples of embodiments of the invention include

1 . Pirfenidone for use in treating a patient in need of pirfenidone therapy, characterized in that the treating comprises avoiding, contraindicating or discontinuing concomitant use of fluvoxamine.

2. The use of pirfenidone in the manufacture of a medicament for treating a patient in need of pirfenidone therapy, characterized in that the treating comprises avoiding, contraindicating or discontinuing concomitant use of fluvoxamine.

3. The pirfenidone of paragraph 1 or use of paragraph 2 wherein the patient is a patient who is avoiding concomitant use of fluvoxamine because concomitant use of pirfenidone with fluvoxamine is contraindicated.

4. The pirfenidone of paragraph 1 or use of paragraph 2 wherein the patient is a patient who has discontinued use of fluvoxamine prior to the initiation of pirfenidone therapy in order to avoid reduced clearance of [or increased exposure to] pirfenidone.

5. Pirfenidone or use of any one of paragraphs 1 to 3, wherein administration of fluvoxamine to the patient is contraindicated or avoided in order to avoid reduced clearance of [or increased exposure to] pirfenidone.

6. The pirfenidone or use of paragraph 4, wherein the patient has discontinued administration of fluvoxamine within 1 month prior to starting pirfenidone therapy.

7. The pirfenidone or use of paragraph 4, wherein the patient has discontinued administration of fluvoxamine within 2 weeks prior to starting pirfenidone therapy.

8. The pirfen idone or use of any one of paragraphs 1 to 7 wherein the patient suffers from a disease selected from pulmonary fibrosis, idiopathic pulmonary fibrosis, idiopathic interstitial pneumonia, autoimmune lung diseases, benign prostate hypertrophy, coronary or myocardial in farction, atrial fibrillation, cerebral infarction, myocardiac fibrosis, musculoskeletal fibrosis, post-surgical adhesions, liver cirrhosis, renal tlbrotic disease, fibrotic vascular disease, scleroderma, Hermansky-Pudlak syndrome, neuro fibromatosis, Alzheimer's disease, diabetic retinopathy, or skin lesions, lymph node fibrosis associated with HIV, chronic obstructive pulmonary disease (COPD), inflammatory pulmonary fibrosis, rheumatoid arthritis; rheumatoid spondylitis; osteoarthritis; gout, other arthritic conditions; sepsis; septic shock; endotoxic shock; gram-negative sepsis; toxic shock syndrome; myo facial pain syndrome (MPS); Shigellosis; asthma; adult respiratory distress syndrome; inflammatory bowel disease; Crohn's disease; psoriasis; eczema; ulcerative colitis; glomerular nephritis; scleroderma; chronic thyroiditis; Grave's disease; Ormond's disease; autoimmune gastritis; myasthenia gravis; autoimmune hemolytic anemia; autoimmune neutropenia; thrombocytopenia; pancreatic fibrosis; chronic active hepatitis including hepatic fibrosis; acute or chronic renal disease; renal fibrosis; diabetic nephropathy; irritable bowel syndrome; pyresis; restenosis; cerebral malaria; stroke or ischemic injury; neural trauma; Alzheimer's disease; Huntington's disease; Parkinson's disease; acute or chronic pain; allergies, including allergic rhinitis or allergic conjunctivitis; cardiac hypertrophy, chronic heart failure; acute coronary syndrome; cachexia; malaria; leprosy; leishmaniasis; Lyme disease; Reiter's syndrome; acute synoviitis; muscle degeneration, bursitis; tendonitis; tenosynoviitis; herniated, ruptured, or prolapsed intervertebral disk syndrome; osteopetrosis; thrombosis; silicosis; pulmonary sarcosis; bone resorption diseases, such as osteoporosis or multiple myeloma-related bone disorders; cancer, including but not limited to metastatic breast carcinoma, colorectal carcinoma, malignant melanoma, gastric cancer, or non-small cell lung cancer; graft-versus-host reaction; or auto-immune diseases, such as multiple sclerosis, lupus or fibromyalgia; AIDS or other viral diseases such as Herpes Zoster, Herpes Simplex I or II, influenza virus, Severe Acute Respiratory Syndrome (SARS) or cytomegalovirus; or diabetes mellitus, proliferative disorders (including both benign or malignant hyperplasias), acute myelogenous leukemia, chronic myelogenous leukemia, Kaposi's sarcoma, metastatic melanoma, multiple myeloma, breast cancer, including metastatic breast carcinoma; colorectal, carcinoma; malignant melanoma; gastric cancer; non- small cell lung cancer (NSCLC); bone metastases; pain disorders including neuromuscular pain, headache, cancer pain, dental pain, or arthritis pain; angiogenic disorders including solid tumor angiogenesis, ocular neovascularization, or infantile hemangioma; conditions associated with the cyclooxygenase or lipoxygenase signaling pathways, including conditions associated with prostaglandin endopcroxide synthase- 2 (including edema, fever, analgesia, or pain); organ hypox ia; thrombin-induced platelet aggregation; or protozoal diseases.

9. The pirfenidone or use of any one o f paragraphs 1 to 7 wherein the patient has Idiopathic Pulmonary Fibrosis (IPF). 10. The pirfenidone or use of any one of paragraphs 1 to 9, wherein the pirfenidone is administered at a total daily dosage of 2400 rag or 2403 mg per day.

1 1. The pirfenidone or use of any one of paragraphs 1 to 10, wherein each dose of pirfenidone administered is 801 mg.

12. The pirfenidone or use of paragraph 1 1 , wherein the pirfenidone is for administration to the patient three times per day, with food.

Other examples of embodiments of the invention include:

1 A. A method of administering pirfenidone therapy to a patient in need thereof, comprising administering to the patient a therapeutically effective amount of pirfenidone, and avoiding administration of fluvoxamine.

2A. The method of paragraph 1 A wherein the patient has idiopathic pulmonary fibrosis (IPF).

3A. The method of paragraph 1 A wherein the therapeutically effective amount of pirfenidone is a daily dosage of 2400 mg or 2403 mg per day.

4A. The method of paragraph 1 A wherein 800 or 801 mg of pirfenidone is administered to the patient three times per day, with food.

5A. A method of administering pirfenidone therapy to a patient in need thereof, comprising discontinuing administration of fluvoxamine to avoid an adverse drug interaction, and administering to the patient a therapeutically effective amount of pirfenidone.

6A. The method of paragraph 5A wherein the patient has idiopathic pulmonary fibrosis (IPF).

7A. The method of paragraph 5A wherein the therapeutically effective amount of pirfenidone is a daily dosage of 2400 mg or 2403 mg per day.

8A. The method of paragraph 5A wherein 800 or 801 mg of pirfenidone is administered to the patient three times per day, with food.

9A. The method of paragraph 5A wherein the fluvoxamine is discontinued within 1 month prior to starling pirfenidone therapy. 10A. The method of paragraph 5A wherein the fluvoxamine is discontinued within 2 weeks prior to starling pirfenidone therapy.

1 1 A, A method of administering pirfenidone therapy to a patient in need thereof, comprising administering to the patient a therapeutically effective amount of pirfenidone, and any one or more o f the following:

(a) advising the patient that fluvoxamine should be avoided or discontinued,

(b) advising the patient that co-administration of pirfenidone with drugs that are moderate to strong inhibitors of both CYP1 A2 and another CYP enzyme selected from the group consisting of CYP2C9, CYP2C19 and CYP3A4 can alter the therapeutic effect or adverse reaction profile of pirfemdone,

(c) advising the patient that co-administration of pirfenidone with fluvoxamine can alter the therapeutic effect or adverse reaction profile of pirfenidone,

(d) advising the patient that use of pirfenidone in patients being treated with fluvoxamine is contraindicated,

(e) advising the patient that co-administration of pirfenidone and fluvoxamine resulted in a 6-fold increase in exposure to pirfenidone, or

f) advising the patient that strong CYP 1 A2 inhibitors should be used with caution in patients receiving pirfenidone due to the potential for reduced pirfenidone clearance.

12A. The method of paragraph 1 1 A wherein the patient is advised that fluvoxamine should be avoided or discontinued.

13A. The method of paragraph 1 1A wherein the patient is advised that coadministration of pirfenidone with drugs that are moderate to strong inhibitors of both CYP 1A2 and another CYP enzyme selected from the group consisting of CYP2C9,

CYP2C 19 and CYP3A4 can alter the therapeutic effect or adverse reaction profile of pirfenidone.

14A. The method of paragraph 1 1 A wherein the patient is advised that coadministration of pirfenidone with fluvoxamine can alter the therapeutic effect or adverse reaction profile of pirfenidone.

15A. The method of paragraph 1 1 A wherein the patient is advised that use of pirfenidone in patients being treated with fluvoxamine is contraindicated. 16 A. The method of paragraph 1 1A wherein the patient is advised that coadministration of pirfenidone and fluvoxamme resulted in a 6-fold increase in exposure to pirfenidone.

1 7A. The method of paragraph 16A further comprising advising the patient that coadministration of pirfenidone and fluvoxamine resulted in a 2-fold increase in average peak serum concentration of pirfenidone (Cmax).

18A. The method of paragraph 1 1 A wherein the patient is advised that strong CYP1 A2 inhibitors should be used with caution in patients receiving pirfenidone due to the potential for reduced pirfenidone clearance.

19A. The method of paragraph 18A further comprising avoiding administering a strong CYP 1 A2 inhibitor.

20A. The method of paragraph 18A further comprising discontinuing administration of a strong CYP 1A2 inhibitor.

Claims

What Is Claimed Is:

1 . Pirfenidone for use i n treating a patient in need of pirfenidone therapy, characterized in that the treating comprises (a) avoiding, contraindicating, discontinuing or using with caution concomitant use or co-administration of a cytochrome P450 1 A2

(CYPl A2) inhibitor that is a moderate to strong inhibitor of both (i) cytochrome P450 1A2 (CYP l A2) and (ii) another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C 19, CYP2B6 and/or CYP2D6, or (b) using with caution pirfenidone in patients receiving a strong inhibitor of CYP 1A2, or (c) using with caution a strong CYP1A2 inhibitor in patients receiving pirfenidone.

2. Use of pirfenidone in preparation of a medicament for treating a patient in need of pirfenidone therapy, characterized in that the treating comprises (a) avoiding, contraindicating, discontinuing or using with caution concomitant use or co-administration of a cytochrome P450 1 A2 (CYPl A2) inhibitor that is a moderate to strong inhibitor of both (i) cytochrome P450 1A2 (CYPl A2) and (ii) another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C 1 , CYP2B6 and/or CYP2D6, or (b) using with caution pirfenidone in patients receiving a strong inhibitor of CYP1A2, or (c) using with caution a strong CYP l A2 inhibitor in patients receiving pirfenidone.

3. A method of administering pirfenidone therapy to a patient in need thereof, comprising administering an effective amount of pirfenidone, and (a) avoiding,

contraindicating, discontinuing or using with caution a cytochrome P450 1 A2 (CYPl A2) inhibitor that is a moderate to strong inhibitor of both (i) cytochrome P450 1 A2 (CYP1A2) and (ii ) another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C 19, CYP2B6 and/or CYP2D6, or (b) using with caution pirfenidone in patients receiving a strong inhibitor of CY l A2, or (c) using with caution a strong CYP 1A2 inhibitor in patients receiving pirfenidone.

4. The pirfenidone, use or method of any of claims 1 -3 wherein the CYPl A2 inhibitor is a moderate to strong inhibitor of CYP1A2 and another CYP enzyme selected from the group consisting of CYP2C9. CYP2C 19 and/or CYP2D6.

5. The pirfenidone, use or method of any of claims 1 -3 herein the CYPl A2 inhibitor is a strong CYP1A2 inhibitor.

6. The pirfenidone, use or method of any of claims 1 -4 wherein the CYPl A2 inhibitor is discontinued prior to starting pirfenidone therapy to avoid an adverse drug interact ion with pirfenidone, or to avoid a reduced clearance of pirfenidone.

7. The pirfenidone of any one of claims 1-6 wherein the CYP1 A2 inhibitor is discontinued within 1 month prior to starting pirfenidone therapy.

8. The pirfenidone of any one of claims 1-7 wherein the CYP 1 A2 inhibitor is discontinued within 2 weeks prior to starting pirfenidone therapy.

9. The pirfenidone, use or method of any of claims 1 -4 wherein the CYP l A2 inhibitor is avoided during pirfenidone therapy.

10. The pirfenidone, use or method of any of claims 1 -9 wherein the patient is in need of therapy with a CYP l A2 inhibitor.

1 1 . The pirfenidone, use or method of any of claims 1 -5 wherein the CYP 1 A2 inhibitor is used with caution.

12. The pirfenidone of any one of claims 1-1 1 wherein the patient has idiopathic pulmonary fibrosis (IPF).

13. The pirfenidone of any of claims 1 -1 1 wherein the patient suffers from a disease selected from idiopathic pulmonary fibrosis, pulmonary fibrosis, , idiopathic interstitial pneumonia, autoimmune lung diseases, benign prostate hypertrophy, coronary or myocardial infarction, atrial fibrillation, cerebral infarction, myocardiac fibrosis, musculoskeletal fibrosis, post-surgical adhesions, liver cirrhosis, renal fibrotic disease, fibrotic vascular disease, scleroderma, Hermansky-Pudlak syndrome, neurofibromatosis, Alzheimer's disease, diabetic retinopathy, or skin lesions, lymph node fibrosis associated with HIV, chronic obstructive pulmonary disease (COPD), inflammatory pulmonary fibrosis, rheumatoid arthritis; rheumatoid spondylitis; osteoarthritis; gout, other arthritic conditions; sepsis; septic shock; endotoxic shock; gram-negative sepsis; toxic shock syndrome;

myofacial pain syndrome (MPS); Shigellosis; asthma; adult respiratory distress syndrome; inflammatory bowel disease; Crohn's disease; psoriasis; eczema; ulcerative colitis;

glomerular nephritis; scleroderma; chronic thyroiditis; Grave's disease; Ormond's disease; autoimmune gastritis; myasthenia gravis; autoimmune hemolytic anemia; autoimmune neutropenia; thrombocytopenia; pancreatic fibrosis; chronic active hepatitis including hepatic fibrosis; acute or chronic renal disease; renal fibrosis; diabetic nephropathy; irritable bow el syndrome; pyresis; restenosis; cerebral malaria; stroke or ischemic injury; neural trauma; Alzheimer's disease; Huntington's disease; Parkinson's disease; acute or chronic pain;

allergies, including allergic rhinitis or allergic conjunctivitis; cardiac hypertrophy, chronic heart failure; acute coronary syndrome; cachexia; malaria; leprosy; leishmaniasis; Lyme disease; Reiter's syndrome; acute synoviitis; muscle degeneration, bursitis; tendonitis: tenosynovitis; herniated, ruptured, or prolapsed intervertebral disk syndrome; osteopetrosis; thrombosis; silicosis; pulmonary sarcosis; bone resorption diseases, such as osteoporosis or multiple myeloma-related bone disorders; cancer, including but not limited to metastatic breast carcinoma, colorectal carcinoma, malignant melanoma, gastric cancer, or non-small cell lung cancer; graft-versus-host reaction; or auto-immune diseases, such as multiple sclerosis, lupus or fibromyalgia; AIDS or other viral diseases such as Herpes Zoster, Herpes Simplex I or II, influenza virus, Severe Acute Respiratory Syndrome (SARS) or

cytomegalovirus; or diabetes mellitus, proliferative disorders (including both benign or malignant hyperplasias), acute myelogenous leukemia, chronic myelogenous leukemia, Kaposi's sarcoma, metastatic melanoma, multiple myeloma, breast cancer, including metastatic breast carcinoma; colorectal, carcinoma; malignant melanoma; gastric cancer; non- small cell lung cancer (NSCLC); bone metastases; pain disorders including neuromuscular pain, headache, cancer pain, dental pain, or arthritis pain; angiogenic disorders including solid tumor angiogenesis, ocular neovascularization, or infantile hemangioma; conditions associated with the cyclooxygenase or lipoxygenase signaling pathways, including conditions associated with prostaglandin endoperoxide synthase-2 (including edema, fever, analgesia, or pain); organ hypoxia; thrombin-induced platelet aggregation; or protozoal diseases.

14. The pirfenidone of any one of claims 1 through 13 wherein the pirfenidone is administered at a total daily dosage of at least 1800 mg.

15. The pirfenidone of any one of claims 1 through 13 wherein the pirfenidone is administered at a total daily dosage of about 2400 mg or 2403 mg.

16. The pirfenidone of any one of claims 1 through 13 wherein 800 or 801 mg of pirfenidone is administered to the patient three times per day, with food.

17. The pirfenidone of any one of claims 1 through 16 wherein the CYP1 A2 inhibitor is fluvoxamine.

18. The pirfenidone of any one of claims 1 through 17 wherein the CYP1 A2 inhibitor is ciprofloxacin, amiodarone or propafenone.

19. The pirfenidone of any one of claims 1 through 16 wherein the CYP1A2 inhibitor is grapefruit juice.

20. A package or kit comprising (a) pirfenidone, optionally in a container, and (b) a package insert, package label, instructions or other labeling comprising avoiding or discontinuing or contraindicating concomitant use of or co-administration of or using with caution (1) a strong inhibitor of CYP1A2, or (2) a moderate to strong inhibitor of both (i ) CYPl A2 and (ii) another CYP enzyme selected from the group consisting of CYP3A4, CYP2C9, CYP2C19, CYP2B6 and/or CYP2D6, optionally according to any of the embodiments of claims 1-19.