EP1003521A1 - Methods to potentiate intravenous estramustine phosphate - Google Patents

Methods to potentiate intravenous estramustine phosphate

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Publication number
EP1003521A1
EP1003521A1 EP99914884A EP99914884A EP1003521A1 EP 1003521 A1 EP1003521 A1 EP 1003521A1 EP 99914884 A EP99914884 A EP 99914884A EP 99914884 A EP99914884 A EP 99914884A EP 1003521 A1 EP1003521 A1 EP 1003521A1
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EP
European Patent Office
Prior art keywords
estramustine
cancer
estramustine phosphate
administered
phosphate
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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Application number
EP99914884A
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German (de)
French (fr)
Other versions
EP1003521A4 (en
Inventor
Michael S. Kopreski
Beryl Asp
Bo Fredholm
Per-Olv Gunnarsson
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Pharmacia and Upjohn Co LLC
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Pharmacia and Upjohn Co
Upjohn Co
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Publication of EP1003521A1 publication Critical patent/EP1003521A1/en
Publication of EP1003521A4 publication Critical patent/EP1003521A4/en
Withdrawn legal-status Critical Current

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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/56Compounds containing cyclopenta[a]hydrophenanthrene ring systems; Derivatives thereof, e.g. steroids
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/08Solutions
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents

Definitions

  • the present invention relates to the use of estramustine phosphate, a non- nitrogen mustard carbamate derivative of estradiol-17b-phosphate. as a high dose infusion.
  • the present invention further relates to methods to potentiate intravenously administered estramustine phosphate and to methods for treating cancer by intravenously administering estramustine phosphate. Discussion of the Background: Cytotoxic effects have been shown to be due to the intact estramustine molecule (Hartley-Asp, 1982). Tissue culture studies have shown that estramustine (EM) is an anti-mitotic agent, causing a dose-dependent blocking of tumor cell division in the metaphase (Hartley-Asp, 1984).
  • Metaphase arrest is known to be caused by an interference of drugs with the microtubule structure that forms the mitotic spindle. It has been shown, with the help of immunohistochemistry. that dose-dependent disturbances of interphase microtubules occur in cultured human prostatic cells (Mareel 1988. Dahllof 1993). Treatment with EM in vitro inhibited the assembly of microtubules composed of only tubulin demonstrating a direct interaction with tubulin (Dahllof 1993). In addition, an interaction with microtubule associated proteins (MAPs) has been demonstrated (Stearns 1988). MAPs are highmolecular weight proteins that are believed to be important in stabilizing microtubules. That EM exhibits the mechanism of action of an anti-mitotic agent has been confirmed in vivo (Ekl ⁇ v. 1992).
  • Estramustine phosphate is thus an anti-mitotic agent currently used in the treatment of advanced adenocarcinoma of the prostate.
  • its activity in hormone-refractory prostate cancer is comparable to that of several other cytotoxic agents that have been studied in a series of multi-institutional, randomized trials by the National Prostatic Cancer Project (Murphy, 1983).
  • the drug is usually administered orally at a dose of 10-15 mg/ kg/day. it is approved for intravenous administration in several countries.
  • estramustine phosphate when administered intravenously has been used at dosages and according to a schedule paralleling the oral administration for the drug, i.e. at recommended dosages of 300- 600 mg daily given intravenously and usually repetitively over for several consecutive days. This is then followed by orally administered drug.
  • estramustine phosphate Phase II trials (Seidman, 1992, Hudes, 1992. Pienta. 1994.
  • estramustine phosphate oral was combined with Etoposide. Fifty two patients were evaluable: including 20 patients with soft tissue disease, in
  • estramustine phosphate appears to be dependent on the presence of the estramustine binding protein (EMBP) (Eklov. 1996). This is found under normal conditions only in the prostate (Forsgren. 1979, Flucher. 1989). However, a similar protein has also been identified in many cancerous tissues, as well as prostate tumors, such as lung, breast glioma. colon, pancreas (Bj ⁇ rk.1991. Bergh 1988. Eklov 1996. Edgren 1996. Von Schoultz. 1994. Bergenheim. 1993).
  • EMBP estramustine binding protein
  • This protein binds estra- and estro-mustine (EaM and EoM) with very high affinity and is thought to be responsible for the selective retention of EoM in the prostate tumor, where a ratio of 1 :6 to 1 : 1 1 plasma/tumor has been found in prostate cancer patients treated with estramustine phosphate oral and intravenously, respectively (Norlen 1988. Walz 1988).
  • EMBP estra- and estro-mustine
  • the present invention describes methods of potentiating the therapeutic use and efficacy of intravenously administered estramustine phosphate It provides for the intravenous administration of estramustine phosphate in dosages exceeding 1300 mg It also provides for intravenous administration of estramustine phosphate at dosages exceeding 950 mg/nr (milligrams per square meter of body surface area) It further provides for administration of high dose intravenous estramustine phosphate as a single dose, which may further be administered on a weekly or longer schedule.
  • the present invention enables optimization of pharmacokinetics as to maximize therapeutic advantage, and further enables use of intravenous estramustine phosphate in combination with other therapies, including other chemotherapies, providing further improved therapeutic benefit
  • the present invention enables use of intravenous estramustine phosphate as therapy for multiple tumor types, including prostate, breast, lung, ovarian, colorectal. melanoma, pancreatic, and brain cancers Thus, one application of the present ⁇ n ⁇
  • Another application is to provide a schedule of intravenous administration, whereby that schedule enables optimization of pharmacokinetics of estramustine phosphate and its metabolites at minimal toxicity. and further wherebv said optimization permits convenient and efficacious combination regimens of therapy
  • an application of the present invention permits the use of intravenous estramustine phosphate in combination with other therapeutic regimens, including cytotoxic chemotherapy
  • Another application of the present inv ention is to provide a method which increases binding saturation and prolongs binding duration of estramustine phosphate or its metabolites to estramustine binding protein or estramustine binding protein-like protein (EMBP).
  • EMBP estramustine binding protein-like protein
  • the present invention provides application to treatment of cancers having EMBP, including but not limited to prostate, breast, lung, ovarian, colorectal. melanoma, pancreatic, and brain cancers, by intravenous administration.
  • cancers having EMBP including but not limited to prostate, breast, lung, ovarian, colorectal. melanoma, pancreatic, and brain cancers, by intravenous administration.
  • Another application of the present invention is to provide a method of rapidly relieving symptoms secondary to cancer, inclusive of but not limited to cancer- induced pain and urinary obstruction. Further, the present invention enables these applications for use of intravenous estramustine phosphate independent of the formulation. Thereby, the present invention provides for the infusion of estramustine phosphate as free drug, as protein- bound drug, or as drug within liposomes.
  • the present invention describes a formulation of estramustine phosphate wherein the estramustine phosphate is administered intravenously in conjunction with liposomes.
  • the method of the present invention in which doses above 900 mg/nr (generally greater than 1300 mg per dose) can be administered safely and within an effective schedule is extremely unexpected.
  • the present invention teaches the advantage of intravenous estramustine in combination with other chemotherapy agents.
  • the present invention further teaches the advantage of high dose intravenous estramustine in combination with other chemotherapeutic agents.
  • intravenous estramustine phosphate may be used to treat tumors having elevated EMBP-like protein (herein referred to simply as EMBP).
  • EMBP EMBP-like protein
  • novel and non-obvious applications of the present invention can be recognized from a comparison of the pharmacokinetic data following oral administration estramustine phosphate with that following high-dose intravenous administration of estramustine phosphate.
  • the pharmacokinetic and toxicity data can be recognized from a comparison of the pharmacokinetic data following oral administration estramustine phosphate with that following high-dose intravenous administration of estramustine phosphate.
  • estromustine EoM
  • estrone analogue of EM are the major metabolic steps after administration of oral estramustine phosphate in man.
  • EoM is the predominant metabolite found in plasma when estramustine phosphate is
  • estromustine is approximately 44%(Gunnarsson. 1984). After intravenous
  • estramustine phosphate is initially found in plasma but is rapidly hydrolyzed to the same metabolites as are found after oral administration, the major
  • estromustine metabolite being estromustine. Both estramustine and estromustine are further
  • estromustine had a half lives of 10-20 hours.
  • the present invention teaches the ability to administer estramustine phosphate at doses above 950 mg/m 1 ( I e , greater than 1300 mg)
  • estramustine phosphate is administered at a single infusion dosage exceeding 950 mg/m 1
  • Intravenous administration is performed either through a central or peripheral intravenous route
  • the contents of packaged estramustine phosphate intended for intravenous usage are dissolved, wherein the packaged contents may consist of but are not limited to a lyophi zed powder of the meglumine salts in vials of estramustine phosphate, oi similar freeze- d ⁇ ed estramustine phosphate which are first dissolved in sterile water such as 5 ml sterile water per 300 mg estramustine phosphate, or in 5% dextrose in water for intravenous administration In the preferred method.
  • estramustine phosphate When estramustine phosphate is administered through a peripheral intravenous route, it is preferred that a longer duration of infusion and greater total infusional volume be utilized to minimize vascular irritation.
  • the estramustine phosphate solution can be mixed with various amounts but preferably 3-5% human albumin or other plasma proteins including synthetic plasma proteins to achieve protein binding of the estramustine phosphate and therefore minimize any potential vascular damage.
  • estramustine phosphate may be further realized using other preparations or formulations of estramustine phosphate.
  • One particularly advantageous preparation of the chemotherapeutic agent estramustine phosphate which enables infusion of estramustine phosphate through either a peripheral or central vein, both at high doses and also doses less than 1300 mg. involves the infusion of estramustine phosphate in conjunction with liposomes (herein referred to as liposome encapsulated estramustine phosphate or liposomal estramustine).
  • liposome encapsulated estramustine phosphate or liposomal estramustine liposomal estramustine.
  • estramustine phosphate solution is first prepared in the manner described above and then injected into a vial containing empty liposomes available as a Ivophilized powder. Following adequate hvdration of the liposomes. the vials are vortexed and sonicated, followed by infusion into the patient.
  • estramustine phosphate When estramustine phosphate is administered through a central venous route, said administration may be performed through either a temporary or permanent venous access device, including but not limited to a triple lumen catheter. Hickman
  • estramustine phosphate in the present invention is greater than 1300 mg, it is preferred that the patient be treated at a dose exceeding 950 mg/nr Thereby, one preferred method is to administer a single intravenous dosage of 1000 mg/m 2 Another preferred method is to administer a single intravenous dosage of 1500 mg/nr Furthermore, a dosage of 2000 mg/nr mav be administered However. the invention is inclusive of other dosages above 950 mg/m 2 and the preferred dosages are not to imply limitation
  • estramustine phosphate administration in the invention is a single infusion given once weekly to a maximal dose of 4000 mg or 3500 mg/m 2
  • Another preferred schedule is administration of a single drug infusion once every two weeks
  • Another preferred schedule is administration of a single drug infusion once ev ery three weeks
  • Another preferred schedule is administration of a single drug infusion once every four weeks
  • One schedule may be preferred over another in consideration of schedules with other concomitant therapy These schedules may repeat in a serial or repetitive fashion.
  • the invention described herein enables methods to prolong blood and/or tissue levels at high elevations tor estramustine phosphate metabolites, including estromustine. estramustine. estrone and estradiol Thereb . enhanced synergistic interactions ith other therapies is enabled, wherein such other therapies include but are not limited to chemotherap . radiotherapy, monoclonal antibodies, and biologic
  • the present invention provides maximization of therapeutic benefit by prolongation of elevated blood and tissue levels of estramustine phosphate and its
  • estramustine phosphate is administered intravenously at dosages exceeding 950 mg/m 2 . which are administered in combination with other cancer therapies, inclusive
  • radiotherapy but not limited to radiotherapy, chemotherapy, monoclonal antibodies, and biologic
  • therapeutic benefit is potentiated by administering intravenous estramustine phosphate at single dosages exceeding 950 mg/nr, with
  • chemotherapeutic agents preferably on the day of, or the day prior to administration
  • the other chemotherapeutic agents consist of anti-mitotic agents or anti-
  • microtubule agents inclusive of but not limited to taxanes. including taxol and
  • taxotere and agents including vinblastine. vincristine, etoposide. navelbine.
  • doxorubicin doxorubicin, irinotecan (CPT-1 1 ). and liposome encapsulated chemotherapeutic
  • liposome encapsulated taxanes such as liposome encapsulated
  • paclitaxel It may be further beneficial if a combination with a monoclonal therapy is utilized, that the monoclonal agent include a radionucleotide or an anti-growth factor agent.
  • Plasma or serum levels of estromustine are further sustained when
  • estramustine phosphate is administered intravenously as a single infusion at a dosage
  • the infusion may optionally be repeated in a serial or repetitive manner to maintain elevated blood levels of the estromustine phosphate metabolites. Sustained levels of estramustine phosphate and its metabolites thereby enable sustained therapeutic benefit.
  • the present invention thereby provides a method to increase the binding saturation of estramustine or its metabolites to estramustine binding protein or like- protein by administering estramustine phosphate intravenously at a single infusion dose exceeding 950 mg/m 2 .
  • the binding duration of estramustine phosphate or its metabolites to estramustine binding protein or estramustine binding protein-like protein (EMBP) is increased in the invention by administering the drug at intravenous dosages exceeding 950 mg/nr.
  • EMBP estramustine binding protein-like protein
  • estramustine phosphate be administered intravenously wherein the single dosage exceeds 950 mg/m 2 when treating cancers having either estramustine binding protein or estramustine binding protein like- protein, inclusive of but not limited to the group of cancers including prostate cancer, breast cancer, ovarian cancer, pancreatic cancer, melanoma, lung cancer, and cancers of the brain.
  • Said cancers may further be treated using liposomal estramustine. either as a single agent or in combination with other chemotherapies.
  • Said administrations are preferably repeated in serial or repetitive fashion at schedules of the invention, with or without combination of other therapies.
  • said schedules may include combinational treatment of intravenous estramustine phosphate with other chemotherapeutic therapies given on a once weekly, a once e ⁇ ery two week, a once every three week, or a once every four week schedule, and variations therein
  • intravenously administered estramustine phosphate be administered in combination with other chemotherapeutic cytotoxic agents when used in the treatment of prostate cancer, breast cancer, melanoma, lung cancer, pancreatic cancer, colorectal cancer, ova ⁇ an.
  • estramustine phosphate be administered in combination with radiation when used in the treatment of prostate cancer, breast cancer, lung cancer, pancreatic cancer, colorectal cancer, and cancers of the brain
  • estramustine phosphate be administered at intravenous dosages exceeding 950 mg/m 2 when used in combination with other cancer therapies
  • the present invention enables both objective and subjective therapeutic benefit Benefit achiev ed may relate to reduction of tumor size, improved quality of life, reduction of tumor obstruction, such as urinary obstruction, reduction of cancer- induced pain, improved survival, reduction in time to cancer recurrence, or other evidence of improvement
  • rapid objectiv e oi subjective therapeutic benefit is achieved bv administering estramustine phosphate intravenously at a dosage exceeding 950 mg/m ⁇ either as a single agent or preferably in combination with other cancer therapies
  • the invention enables rapid relief of cancer-induced urinary obstruction, and rapid relief of cancer-induced pain
  • Example 1 Two patients with advanced metastatic prostate cancer were treated with estramustine phosphate intravenously given through a central line. The
  • phosphate was administered as a single infusion on a weekly schedule in a repetitive
  • PSA prostate specific antigen
  • Example 2 Three patients with advanced metastatic prostate cancer were
  • Estramustine phosphate was administered as a single infusion on a weekly schedule in a repetitive fashion. Each infusional dose was
  • Example 3 Three patients with advanced metastatic prostate cancer were treated with estramustine phosphate administered intravenously through a central line at a dosage of 1500 mg/m 2 . Estramustine phosphate was administered as a single infusion on a weekly schedule in a repetitive fashion. The infusional dose was administered either over 30 minutes or over 1 hour. The infusions were well tolerated with one patient demonstrating a response in bulky tumor adenopathy.
  • Example 4 Three patients with advanced metastatic prostate cancer were treated with estramustine phosphate intravenously given through a central line. The patients received an estramustine phosphate dosage of 2000 mg/m 2 . Estramustine phosphate was administered as a single infusion on a weekly schedule in a repetitive fashion. Each infusional dose was administered over a 60 minute infusion. An anti- thrombotic agent was additionally administered for venous thrombosis prophylaxis.
  • estramustine phosphate infusions were well tolerated without serious toxicity, and with evidence of PSA response.
  • Ekl ⁇ v S. Mahdy E, Wester K et al. Estramustine-binding protein (EMBP) content in four different cell lines and its correlation to estramustine induced metaphase arrest.
  • Fl ⁇ chter S. Nelde HJ. Bj ⁇ rk P et al. Effect of treatment on the expression of estramustine-binding protein (EMBP) in prostatic cancer patients: An immunohistochemical study. The Prostate 14:27-43, 1989
  • Mareel MM Storme GA. Dragonetti CH. De Bruyne GK. Hartley-Asp B, Segers JL. Rabaey ML. Antiinvasive activity of estramustine on malignant MO,
  • Nagel R, K ⁇ lln C-P Treatment of advanced carcinoma of the prostate with
  • Petrylak DP Shelton GB. Mac Arthur RB et al.: Phase I trial of Docetaxel -
  • Tew KD Estramustine binds MAP-2 to inhibit microtubule

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Abstract

Estramustine phosphate is an anti-mitotic chemotherapeutic drug with proven efficacy against cancer. The invention describes methods which potentiate the therapeutic benefit of intravenous estramustine phosphate. The invention provides for intravenous estramustine phosphate to be administrated at a high dosage exceeding 1300 mg as a single dose. Efficacious enhancement of estramustine phosphate pharmacokinetics is thereby achieved. Further provided, estramustine phosphate may be intravenously administered for use in combinational regimens with other chemotherapeutic agent. The therapeutic advantages achieved using the intravenous estramustine phosphate formulation are applicable to treatment of a variety of cancers including prostate cancer, breast cancer, lung cancer, colorectal cancer, pancreatic cancer, ovarian cancer, melanoma, and other cancers.

Description

TITLE OF THE INVENTION
METHODS TO POTENTIATE INTRAVENOUS ESTRAMUSTINE PHOSPHATE This application claims priority to U. S. Provisional Application serial No.
60/079.542. which was filed on March 27. 1998.
BACKGROUND OF THE INVENTION Field of the Invention:
The present invention relates to the use of estramustine phosphate, a non- nitrogen mustard carbamate derivative of estradiol-17b-phosphate. as a high dose infusion. The present invention further relates to methods to potentiate intravenously administered estramustine phosphate and to methods for treating cancer by intravenously administering estramustine phosphate. Discussion of the Background: Cytotoxic effects have been shown to be due to the intact estramustine molecule (Hartley-Asp, 1982). Tissue culture studies have shown that estramustine (EM) is an anti-mitotic agent, causing a dose-dependent blocking of tumor cell division in the metaphase (Hartley-Asp, 1984). Metaphase arrest is known to be caused by an interference of drugs with the microtubule structure that forms the mitotic spindle. It has been shown, with the help of immunohistochemistry. that dose- dependent disturbances of interphase microtubules occur in cultured human prostatic cells (Mareel 1988. Dahllof 1993). Treatment with EM in vitro inhibited the assembly of microtubules composed of only tubulin demonstrating a direct interaction with tubulin (Dahllof 1993). In addition, an interaction with microtubule associated proteins (MAPs) has been demonstrated (Stearns 1988). MAPs are highmolecular weight proteins that are believed to be important in stabilizing microtubules. That EM exhibits the mechanism of action of an anti-mitotic agent has been confirmed in vivo (Eklδv. 1992).
Estramustine phosphate is thus an anti-mitotic agent currently used in the treatment of advanced adenocarcinoma of the prostate. As a single agent, its activity in hormone-refractory prostate cancer is comparable to that of several other cytotoxic agents that have been studied in a series of multi-institutional, randomized trials by the National Prostatic Cancer Project (Murphy, 1983). While the drug is usually administered orally at a dose of 10-15 mg/ kg/day. it is approved for intravenous administration in several countries. However, estramustine phosphate when administered intravenously has been used at dosages and according to a schedule paralleling the oral administration for the drug, i.e. at recommended dosages of 300- 600 mg daily given intravenously and usually repetitively over for several consecutive days. This is then followed by orally administered drug.
In the published material, details from about 500 patients who have been treated with the intravenous formulation initially which was then followed by oral treatment can be found. Induction schedules employing 300-600 mg intravenous daily for 7-21 days, followed by daily oral doses, were typical in these studies. The drug was administered as a slow intravenous injection or as a bolus at 300 mg/day. and thrombophlebitis and local irritation at the peripheral intravenous injection sites were considered major limitations of drug administration requiring the establishment of central line administration in many patients or discontinuation of treatment. At 450 mg/day. Nagel and Kόlln ( 1977) stated that this led to so "severe gastrointestinal problems that 300 mg/day was taken as the maximum intravenous daily- dose." In a compilation, by Andersson et al. of 245 patients receiving 300-600 mg /day for 21 days followed by the same dose once or twice weekly for 2 months. 20% of the patients exhibited thrombophlebitis. 17% exhibited gastrointestinal problems and 9% exhibited liver disturbances. Toxicities resulting from such repetitive dosing schedules often require drug discontinuation (Lundgren. 1995). Maier ( 1990), administered daily intravenous doses of 900 mg/day for 7-10 days, followed by oral therapy, without reporting phlebitis but severe liver problems did occur in 1 1 of 18 patients (61%) with one death due to toxic liver failure. The state of the art thus typically utilized intravenous estramustine phosphate formulations as a single-agent method for initiating a long term oral estramustine therapy. Furthermore, intravenous administration of estramustine phosphate at higher dosages is generally considered prohibitive due to toxicity. It is neither known nor obvious to the art that single dose, high-dosage administration of estramustine phosphate is feasible intravenously. While dosing up to 1200 mg/nr have been given orally (Keren-Rosenberg. 1 97). differences in drug metabolism and bioavailability do not permit extrapolation to the high dose intravenous formulation, with relative bioavailability of estromustine after oral administration found to be only 44%. (Gunnarsson. 1984). with the phosphate moiety dephosphorylated in the oral formulation in contrast to the intravenous formulation. Furthermore, it is not known in the art that intravenous estramustine phosphate can be used in combinational chemotherapy regimens, including the use of higher dose intravenous estramustine phosphate. Furthermore, it is not known to the art that intravenous estramustine phosphate has clinical utility for cancers other than for the prostate cancer indication. In previous work. Dr. Beryl Hartley-Asp. a co-inventor of this invention, was
the first to recognize the synergistic potential of estramustine phosphate with other
cytotoxic agents. (Mareel 1988). In several experiments, it was demonstrated that prolonged exposure to estramustine was necessary to achieve potentiation. Consequently, daily dosing was deemed necessary leading to the use of the ORAL preparation as previous data from the intravenous (IV) preparation suggested that
achievement of constant high levels would not be clinically achievable with IV
dosing.
Additive and possibly synergistic antimicrotubule effects in cells in vitro have
been shown for estramustine and many other cytotoxic agents, (Mareel 1988. Speicher
1992. Pienta 1993, Batra, 1996). Thus, the combination of estramustine phosphate with other drugs in humans has been carried out using ORAL administration of
estramustine phosphate. Phase II trials (Seidman, 1992, Hudes, 1992. Pienta. 1994.
Hudes, 1996) with Estramustine phosphate combined with vinblastme. have been carried out in hormone refractory prostate cancer. In these trials a 50-75% decrease in prostate specific antigen was demonstrated among 88 patients. The most frequent
toxicity was mild to moderate nausea. Of particular note is the 10.5% (4/37)
incidence of significant cardiovascular toxicity including one deep venous thrombosis
(DVT), one myocardial infarction, one episode of congestive heart failure, and one
reversible neurologic event which required stopping therapy in these patients and
which can be attributed to estramustine phosphate. In another Phase II trial carried out
by Pienta et al ( 1994). estramustine phosphate (oral) was combined with Etoposide. Fifty two patients were evaluable: including 20 patients with soft tissue disease, in
which 3 complete responses (CR) ( 15%) and 6 partial responses (PR) (30%) were observed. In 32 patients with bone metastases 8 patients improved (25%), and 12 patients were stable (38%). Overall 13 men (25%) had a 75% decrease in prostate specific antigen, and 28 men ( 54%) had a 50% decrease. A Phase I-II study of Taxol (Hudes. 1992) and estramustine phosphate was carried out in seventeen patients with hormone refractory prostate cancer. Six patients had measurable disease and 3 of these obtained a PR of 2+. 6. and 8 months. Prostate specific antigen (PSA) decreased by ^ 50% in 58.8%. Median duration of response was 7 months. Grade 3- 4 granulocytopenia and mucositis occurred in 2 patients, nausea grade 1-2 (70.5%) and grade 3 in one patient. Edema was seen in 8 patients (47%) and transient hepatic enzyme elevation of grade 1 -3 in 6 patients (35.2%).
In a recent study, Petrylak et al., (1997), using escalating doses of docetaxel with estramustine phosphate given orally demonstrated an overall prostate specific antigen response rate of 62%. In patients with bidimensionally measurable disease. 3 (43%o) achieved a partial response in lymph nodes, and 1 achieved a minor response in ischial mass. This demonstrates that combination treatment with ORAL estramustine phosphate is efficacious. However, combinations of intravenous estramustine phosphate with these cytotoxic agents are not known to the art. Differences in the metabolism, particularly regarding the phosphate moiety, in the oral versus intravenous estramustine phosphate formulations make combinational therapies with the intravenous formulation non-obvious.
In contrast to other anti-mitotic agents, the effect of estramustine phosphate appears to be dependent on the presence of the estramustine binding protein (EMBP) (Eklov. 1996). This is found under normal conditions only in the prostate (Forsgren. 1979, Flucher. 1989). However, a similar protein has also been identified in many cancerous tissues, as well as prostate tumors, such as lung, breast glioma. colon, pancreas (Bjδrk.1991. Bergh 1988. Eklov 1996. Edgren 1996. Von Schoultz. 1994. Bergenheim. 1993). This protein binds estra- and estro-mustine (EaM and EoM) with very high affinity and is thought to be responsible for the selective retention of EoM in the prostate tumor, where a ratio of 1 :6 to 1 : 1 1 plasma/tumor has been found in prostate cancer patients treated with estramustine phosphate oral and intravenously, respectively (Norlen 1988. Walz 1988). Recently, we have demonstrated a correlation between the levels of EMBP and the levels ofEaM and EoM in human prostate tumors after a single intravenous estramustine phosphate dose to patients before radical prostatectomy, indicating that EMBP could be the cause of drug retention
(Walz. 1996).
BRIEF DESCRIPTION OF THE FIGURES A more complete appreciation of the invention and many of the attendant advantages thereof will be readily obtained as the same become better understood by reference to the following detailed description when considered in connection with the accompanying drawings, wherein:
Figure 1 illustrates the concentration of estramustine phosphate after a single intravenous dose of Estracyt (mean ± SEM. N = 4 + 4 + 3) given at a dosage of 1000 mg (range 980-1070 mg), 1000 mg/nr. and 1500 mg/nr; and Figure 2 illustrates the concentration of estromustine after a single intravenous dose of Estracyt (mean ± SEM. n = 4 + 4 + 3) given at a dosage of 1000 mg (range 980-1070 mg), 1000 mg/nr. and 1500 mg/nr. SUMMARY OF THE INVENTION The present invention describes methods of potentiating the therapeutic use and efficacy of intravenously administered estramustine phosphate It provides for the intravenous administration of estramustine phosphate in dosages exceeding 1300 mg It also provides for intravenous administration of estramustine phosphate at dosages exceeding 950 mg/nr (milligrams per square meter of body surface area) It further provides for administration of high dose intravenous estramustine phosphate as a single dose, which may further be administered on a weekly or longer schedule The present invention enables optimization of pharmacokinetics as to maximize therapeutic advantage, and further enables use of intravenous estramustine phosphate in combination with other therapies, including other chemotherapies, providing further improved therapeutic benefit The present invention enables use of intravenous estramustine phosphate as therapy for multiple tumor types, including prostate, breast, lung, ovarian, colorectal. melanoma, pancreatic, and brain cancers Thus, one application of the present ιn\ ention is to provide high dose estramustine phosphate therapy intravenoush wherein the dose exceeds 950 mg/nr
Another application is to provide a schedule of intravenous administration, whereby that schedule enables optimization of pharmacokinetics of estramustine phosphate and its metabolites at minimal toxicity. and further wherebv said optimization permits convenient and efficacious combination regimens of therapy
Thus, an application of the present invention permits the use of intravenous estramustine phosphate in combination with other therapeutic regimens, including cytotoxic chemotherapy
Another application of the present inv ention is to provide a method which increases binding saturation and prolongs binding duration of estramustine phosphate or its metabolites to estramustine binding protein or estramustine binding protein-like protein (EMBP).
Thereby, the present invention provides application to treatment of cancers having EMBP, including but not limited to prostate, breast, lung, ovarian, colorectal. melanoma, pancreatic, and brain cancers, by intravenous administration.
Another application of the present invention is to provide a method of rapidly relieving symptoms secondary to cancer, inclusive of but not limited to cancer- induced pain and urinary obstruction. Further, the present invention enables these applications for use of intravenous estramustine phosphate independent of the formulation. Thereby, the present invention provides for the infusion of estramustine phosphate as free drug, as protein- bound drug, or as drug within liposomes.
Thereby, the present invention describes a formulation of estramustine phosphate wherein the estramustine phosphate is administered intravenously in conjunction with liposomes.
Thus, the method of the present invention in which doses above 900 mg/nr (generally greater than 1300 mg per dose) can be administered safely and within an effective schedule is extremely unexpected. The present invention teaches the advantage of intravenous estramustine in combination with other chemotherapy agents. The present invention further teaches the advantage of high dose intravenous estramustine in combination with other chemotherapeutic agents.
We teach in this invention that intravenous estramustine phosphate may be used to treat tumors having elevated EMBP-like protein (herein referred to simply as EMBP).
The novel and non-obvious applications of the present invention can be recognized from a comparison of the pharmacokinetic data following oral administration estramustine phosphate with that following high-dose intravenous administration of estramustine phosphate. The pharmacokinetic and toxicity data
regarding high-dose intravenous estramustine phosphate is not known to the art.
Dephosphorylation of estramustine phosphate to estramustine (EM), followed by
oxidation at the 17 position to estromustine ( EoM). the estrone analogue of EM. are the major metabolic steps after administration of oral estramustine phosphate in man.
EoM is the predominant metabolite found in plasma when estramustine phosphate is
administered on the daily oral schedule. The relative bioavailability based on
estromustine is approximately 44%(Gunnarsson. 1984). After intravenous
administration estramustine phosphate is initially found in plasma but is rapidly hydrolyzed to the same metabolites as are found after oral administration, the major
metabolite being estromustine. Both estramustine and estromustine are further
metabolized by cleavage of the carbamic ester to yield approximately 15%) estradiol and estrone. respectively (Gunnarsson, 1981. 1984). We have demonstrated an
unexpected prolonged availability of the major metabolite estromustine following high-dose intravenous administration, which can lead to unexpected clinical benefits.
Previous data from patients treated with a single intravenous dose of 300 mg
demonstrated that the elimination of estromustine had a half lives of 10-20 hours. The
main route of elimination was metabolism of estromustine phosphate to estramustine, estromustine, estradiol and estrone. The data of particular importance for the efficacy of estramustine phosphate was the half lives of estramustine phosphate. (Figure 1), and the major cvtotoxic metabolite estromustine (Figure 2) Bv application of the methods of this inv ention. we now demonstrate the novel finding that after a single high intravenous dose of estramustine phosphate at lOOOmg nr it was found that the half life of estromustine was approximately 100 hours (Figure 2) This finding further enables therapeutic applications of high-dose intravenous estramustine phosphate
DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS The present invention teaches the ability to administer estramustine phosphate at doses above 950 mg/m1 ( I e , greater than 1300 mg)
The method of the present invention is performed as follows In the preferred method, estramustine phosphate is administered at a single infusion dosage exceeding 950 mg/m1 Intravenous administration is performed either through a central or peripheral intravenous route During preparation of the intended drug, the contents of packaged estramustine phosphate intended for intravenous usage are dissolved, wherein the packaged contents may consist of but are not limited to a lyophi zed powder of the meglumine salts in vials of estramustine phosphate, oi similar freeze- dπed estramustine phosphate which are first dissolved in sterile water such as 5 ml sterile water per 300 mg estramustine phosphate, or in 5% dextrose in water for intravenous administration In the preferred method. 5% dextrose in water is used as the diluent In the preferred method, during preparation of the dissolved drug the preparation should not be shaken, but should be slowh inverted to mix The solution is then given as an intrav enous infusion with the preferred duration of infusion time
10 being 30 minutes to 3 hours, whereby infusion over 1-2 hours is a safe and convenient method. Saline solution may result in drug precipitation and thereby its use is not preferred in the infusion.
When estramustine phosphate is administered through a peripheral intravenous route, it is preferred that a longer duration of infusion and greater total infusional volume be utilized to minimize vascular irritation. Alternatively, the estramustine phosphate solution can be mixed with various amounts but preferably 3-5% human albumin or other plasma proteins including synthetic plasma proteins to achieve protein binding of the estramustine phosphate and therefore minimize any potential vascular damage.
The invention may be further realized using other preparations or formulations of estramustine phosphate. One particularly advantageous preparation of the chemotherapeutic agent estramustine phosphate which enables infusion of estramustine phosphate through either a peripheral or central vein, both at high doses and also doses less than 1300 mg. involves the infusion of estramustine phosphate in conjunction with liposomes (herein referred to as liposome encapsulated estramustine phosphate or liposomal estramustine). In one preferred method of preparing liposomal estramustine, estramustine phosphate solution is first prepared in the manner described above and then injected into a vial containing empty liposomes available as a Ivophilized powder. Following adequate hvdration of the liposomes. the vials are vortexed and sonicated, followed by infusion into the patient.
When estramustine phosphate is administered through a central venous route, said administration may be performed through either a temporary or permanent venous access device, including but not limited to a triple lumen catheter. Hickman
1 1 catheter, subclavian line, jugular line, or medi-port. Said administration may be but is not necessarily performed concomitant with anticoagulant therapy or with the addition of varying amounts but preferably 3-5% human albumin or other plasma proteins or liposomal estramustine to minimize any potential vascular damage in a given patient. While the dosage of estramustine phosphate in the present invention is greater than 1300 mg, it is preferred that the patient be treated at a dose exceeding 950 mg/nr Thereby, one preferred method is to administer a single intravenous dosage of 1000 mg/m2 Another preferred method is to administer a single intravenous dosage of 1500 mg/nr Furthermore, a dosage of 2000 mg/nr mav be administered However. the invention is inclusive of other dosages above 950 mg/m2 and the preferred dosages are not to imply limitation
The most preferred schedule of estramustine phosphate administration in the invention is a single infusion given once weekly to a maximal dose of 4000 mg or 3500 mg/m2 Another preferred schedule is administration of a single drug infusion once every two weeks Another preferred schedule is administration of a single drug infusion once ev ery three weeks Another preferred schedule is administration of a single drug infusion once every four weeks One schedule may be preferred over another in consideration of schedules with other concomitant therapy These schedules may repeat in a serial or repetitive fashion. The invention described herein enables methods to prolong blood and/or tissue levels at high elevations tor estramustine phosphate metabolites, including estromustine. estramustine. estrone and estradiol Thereb . enhanced synergistic interactions ith other therapies is enabled, wherein such other therapies include but are not limited to chemotherap . radiotherapy, monoclonal antibodies, and biologic
12 therapies. The present invention provides maximization of therapeutic benefit by prolongation of elevated blood and tissue levels of estramustine phosphate and its
metabolites. Thereby, maximization of therapeutic benefit is achieved wherein estramustine phosphate is administered intravenously at dosages exceeding 950 mg/m2. which are administered in combination with other cancer therapies, inclusive
but not limited to radiotherapy, chemotherapy, monoclonal antibodies, and biologic
therapies.
In the preferred method, therapeutic benefit is potentiated by administering intravenous estramustine phosphate at single dosages exceeding 950 mg/nr, with
other cytotoxic chemotherapies. In the preferred method said combination is achieved by administering intravenous estramustine phosphate within 3 days of the other
chemotherapeutic agents, preferably on the day of, or the day prior to administration
of the other chemotherapeutic agents. A particularly preferred method is achieved when the other chemotherapeutic agents consist of anti-mitotic agents or anti-
microtubule agents, inclusive of but not limited to taxanes. including taxol and
taxotere. and agents including vinblastine. vincristine, etoposide. navelbine.
doxorubicin, irinotecan (CPT-1 1 ). and liposome encapsulated chemotherapeutic
agents, including liposome encapsulated taxanes such as liposome encapsulated
paclitaxel. It may be further beneficial if a combination with a monoclonal therapy is utilized, that the monoclonal agent include a radionucleotide or an anti-growth factor agent.
Plasma or serum levels of estromustine are further sustained when
estramustine phosphate is administered intravenously as a single infusion at a dosage
exceeding 950 mg/m2. The infusion may optionally be repeated in a serial or repetitive manner to maintain elevated blood levels of the estromustine phosphate metabolites. Sustained levels of estramustine phosphate and its metabolites thereby enable sustained therapeutic benefit.
The present invention thereby provides a method to increase the binding saturation of estramustine or its metabolites to estramustine binding protein or like- protein by administering estramustine phosphate intravenously at a single infusion dose exceeding 950 mg/m2. Similarly, the binding duration of estramustine phosphate or its metabolites to estramustine binding protein or estramustine binding protein-like protein (EMBP) is increased in the invention by administering the drug at intravenous dosages exceeding 950 mg/nr. Thereby, all cancers having either estramustine binding protein or estramustine binding protein like-protein may be treated by intravenous estramustine phosphate. It is particularly preferred to treat prostate cancer in such manner. It is further preferred to treat breast cancer, melanoma, lung cancer, pancreatic cancer, colorectal cancer, ovarian cancer, and cancers of the brain in such manner. It is particularly preferred that estramustine phosphate be administered intravenously wherein the single dosage exceeds 950 mg/m2 when treating cancers having either estramustine binding protein or estramustine binding protein like- protein, inclusive of but not limited to the group of cancers including prostate cancer, breast cancer, ovarian cancer, pancreatic cancer, melanoma, lung cancer, and cancers of the brain.
Said cancers may further be treated using liposomal estramustine. either as a single agent or in combination with other chemotherapies. Said administrations are preferably repeated in serial or repetitive fashion at schedules of the invention, with or without combination of other therapies. Thus, said schedules may include combinational treatment of intravenous estramustine phosphate with other chemotherapeutic therapies given on a once weekly, a once e\ ery two week, a once every three week, or a once every four week schedule, and variations therein It is particularlv preferred that intravenously administered estramustine phosphate be administered in combination with other chemotherapeutic cytotoxic agents when used in the treatment of prostate cancer, breast cancer, melanoma, lung cancer, pancreatic cancer, colorectal cancer, ovaπan. and cancers of the brain. It is further particularlv preferred that intravenously administered estramustine phosphate be administered in combination with radiation when used in the treatment of prostate cancer, breast cancer, lung cancer, pancreatic cancer, colorectal cancer, and cancers of the brain It is further preferred that in treating cancers having estramustine binding protein or estramustine binding protein like-protein, including prostate cancer, breast cancer, lung cancer, pancreatic cancer, colorectal cancer, ovarian cancer, and cancers of the brain, estramustine phosphate be administered at intravenous dosages exceeding 950 mg/m2 when used in combination with other cancer therapies
The present invention enables both objective and subjective therapeutic benefit Benefit achiev ed may relate to reduction of tumor size, improved quality of life, reduction of tumor obstruction, such as urinary obstruction, reduction of cancer- induced pain, improved survival, reduction in time to cancer recurrence, or other evidence of improvement In particular, rapid objectiv e oi subjective therapeutic benefit is achieved bv administering estramustine phosphate intravenously at a dosage exceeding 950 mg/m\ either as a single agent or preferably in combination with other cancer therapies Therebv the invention enables rapid relief of cancer-induced urinary obstruction, and rapid relief of cancer-induced pain
15 Other features of the invention will become apparent in the course of the
following descriptions of exemplary embodiments which are given for illustration of the invention and are not intended to be limiting thereof.
EXAMPLES The following clinical cases are provided by way of example and not
limitation.
Example 1 : Two patients with advanced metastatic prostate cancer were treated with estramustine phosphate intravenously given through a central line. The
patients received an estramustine phosphate dosage of 2500 mg/nr. Estramustine
phosphate was administered as a single infusion on a weekly schedule in a repetitive
fashion. Each infusional dose was administered over a 90 minute infusion. The
infusions were well tolerated without serious toxicity and both patients demonstrated a response (reduction) in their prostate specific antigen (PSA).
Example 2: Three patients with advanced metastatic prostate cancer were
treated with estramustine phosphate administered intravenously through a central line
at a dosage of 1000 mg/m2. Estramustine phosphate was administered as a single infusion on a weekly schedule in a repetitive fashion. Each infusional dose was
administered over a 30 minute infusion. The infusions were well tolerated with
several patients demonstrating PSA response.
Example 3 : Three patients with advanced metastatic prostate cancer were treated with estramustine phosphate administered intravenously through a central line at a dosage of 1500 mg/m2. Estramustine phosphate was administered as a single infusion on a weekly schedule in a repetitive fashion. The infusional dose was administered either over 30 minutes or over 1 hour. The infusions were well tolerated with one patient demonstrating a response in bulky tumor adenopathy.
Example 4: Three patients with advanced metastatic prostate cancer were treated with estramustine phosphate intravenously given through a central line. The patients received an estramustine phosphate dosage of 2000 mg/m2. Estramustine phosphate was administered as a single infusion on a weekly schedule in a repetitive fashion. Each infusional dose was administered over a 60 minute infusion. An anti- thrombotic agent was additionally administered for venous thrombosis prophylaxis.
The estramustine phosphate infusions were well tolerated without serious toxicity, and with evidence of PSA response.
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Batra S. Karlsson R. Witt L: Potentiation by estramustine of the cytotoxic effect of vinblastine and doxorubicin in prostatic tumor cells, h t J Cancer 68: 1-6. 1996 Bergenheim AT. Gunnarsson PO, Edman K. von Schoultz E. Hariz MI
Henriksson R: Uptake and retention of estramustine and the presence of estramustine binding protein in malignant brain tumors in humans. Br .1 Cancer 67:358-361. 1993
17 Bergh J, Bjόrk P. Westlin J-E. Nilsson S: Expression of an Estramustine- binding associated protein in human lung cancer cell lines. Cancer Res 48:4615-4619, 1988
Bjόrk P, Borg A, Fernδ M. Nilsson S: Expression and partial characterization of estramustine-binding protein (EMBP) in human breast cancer and malignant melanoma. Anticancer Res 1 1(3):1 173-1 182. 1991
Bjόrk P. Jδnsson U. Andren-Sandberg A: Binding sites for the cytotoxic metabolites of Estramustine phosphate (Estracyt®) in rat and human pancreas that are distinct from pancreatic Estrogen-binding protein. Pancreas 6: 1 :77-89. 1991 Dahllof B. Hartley-Asp B. Billstrόm A, Cabral F: Estramustine depolymerizes microtubules by binding to tubulin. Cancer Res 53:4573-4581. 1993
Edgren M, Westlin JE. Letocha H et al.: Estramustine-binding protein (EMBP) in renal cell carcinoma immunohistochemistry, immunoscintigraphy and in vitro estramustine effects. Acta Oncol 35(4):483-488, 1996 Eklδv S et al., Evidence for a non-estrogenic cytostatic effect of estramustine on human prostatic carcinoma cells in vivo. The Prostate 20:43-50. 1992
Eklδv S. Mahdy E, Wester K et al.: Estramustine-binding protein (EMBP) content in four different cell lines and its correlation to estramustine induced metaphase arrest. Anticancer Res 16(4A): 1819-1822. 1996 Flϋchter S. Nelde HJ. Bjόrk P et al.: Effect of treatment on the expression of estramustine-binding protein (EMBP) in prostatic cancer patients: An immunohistochemical study. The Prostate 14:27-43, 1989
Forsgren B. Bjόrk P. Carlstrόm K. Gustafsson JA. Pousette A. Hόgberg B: Purification and distribution of a major protein in rat prostate that binds estramustine.
18 a nitrogen mustard derivative of estradiol- 17β. Proc. Natl. Acad. Sci USA: 76:3149- 3153, 1979
Gunnarsson PO. Andersson S-B. Johansson S-A et al.: Pharmacokinetics of estramustine phosphate (Estracyt®) in prostatic cancer patients. Eur J Clin Pharmacol 26: 1 13-1 19. 1984
Gunnarsson PO. Plym Forshell G. Fritjofsson A. Norlen BJ: Plasma concentration of Estramustine phosphate and its major metabolites in patients with prostatic carcinoma treated with different doses of Estramustine phosphate (Estracyt®). Scand J Urol Nephrol 15:201-206. 1981 Hartley-Asp B: Estramustine induced mitotic arrest in two human prostatic carcinoma cell lines DU 145 and PC-3. The Prostate 5:93-100. 1984
Hartley-Asp B. Gunnarsson PO: Growth and cell survival following treatment with estramustine, nor-nitrogen mustard, estradiol and testosterone of a human prostatic cancer cell line (DU 145). J Urology 127:818-822, 1982 Hudes G, Obasaju C. Chapman A, Gallo J. McAleer C, Greenberg R: Phase I study of Paclitaxel and Estramustine: Preliminary activity in hormone refractory prostate cancer. Sem Oncol. Vol 22:3. Suppl 6:6-1 1, 1995
Hudes GR, Greenberg R. Krigel RL, Fox S. et al.: Phase II study of estramustine and vinblastine. two microtubule inhibitors, in hormone-refractory prostate cancer. J Clin Oncol 10: 1754-1761. 1992
Keren-Rosenberg, S. Muggia. FM: Response to estramustine phosphate and paclitaxel in patients with advanced breast cancer: A phase I Study Seminars in Oncology 24:5 S3-26 - S3-29. 1997
Lindberg B: Treatment of rapidly progressing prostatic carcinoma with Estracyt. Journal of Urol 108:303-305. 1972
Maier U. Hienert G. Simak R: Estramustine phosphate in secondary hormone- resistant carcinoma of the prostate. Eur Urol 17:216-218. 1990
Mareel MM. Storme GA. Dragonetti CH. De Bruyne GK. Hartley-Asp B, Segers JL. Rabaey ML. Antiinvasive activity of estramustine on malignant MO,
mouse cells and DU 145 human prostate carcinoma cells in vitro. Cancer Res
48: 1842-1849, 1988
Murphy GP. Slack NH. Mittleman A: Experiences with Estramustine Phosphate (Estracyt. Emcyt) in prostate cancer. Seminars in oncology 10(3) Suppl 3. 34-42. 1983
Nagel R, Kδlln C-P: Treatment of advanced carcinoma of the prostate with
estramustine phosphate. British Journal of Urol 49:73-79, 1977
Norlen, B.J.. Andersson S.B., Bjόrk P., Gunnarsson P.O., Fritjofsson A.
Uptake of Estramustine phosphate (Estracyt) metabolites in prostate cancer. Journal of
Urology 140: 1058- 1062. 1988
Petrylak DP. Shelton GB. Mac Arthur RB et al.: Phase I trial of Docetaxel -
Estramustine in androgen insensitive prostate cancer. Cancer Investigation 16. Supp 1 p 62. 1997
Pienta KJ. Lehr JE: Inhibition of prostate cancer growth by estramustine and etoposide: Evidence for interaction at the nuclear matrix. Journal of Urol 149: 1622-
1625. 1993
Pienta KJ. Redman B. Hussain M, Cummings G et al.: Phase II evaluation of oral estramustine and oral etoposide in hormone-refractory adenocarcinoma of the prostate. J Clin Oncol 12:2005-2012. 1994
20 Seidman AD. Scher HI. Petrylak D. Dershaw DD. Curley T: Estramustine and vinblastine: Use of prostate specific antigen as a clinical trial end point for hormone refractory prostatic cancer. J Urol 147:93 1 -934. 1992
Speicher LA, Barone L. Tew KD: Combined antimicrotubule activity of
estramustine and Taxol in human prostatic carcinoma cell lines. Cancer Res 52:4433-
4440. 1992
Stearns M. Tew KD: Estramustine binds MAP-2 to inhibit microtubule
assembly in vitro. J Cell Science 89:33 1 -342. 1988 von Schoultz E. Carlstrόm K. Henriksson R et al.: Estramustine binding
protein in primary tumors and metastases of malignant melanoma. Melanoma Res
4(6):401 -405, 1994
Walz PH. Bjόrk P, Edman K, Gunnarsson PO, Hartley- Asp B: Uptake and distribution of the estramustine-phosphate metabolite estramustine after single-dose
injection in patients with prostatic cancer. Akt Urol 27:92-93, 1996
Lundgren. R. Estracyt intravenost for behandling av
hormonreftraktarprostatacancer: Svenska Lakaresallskapets Rikstamma. 1995
This application is based on U. S. Provisional Application serial No. 60/079.542. which was filed on March 27. 1998. which is incorporated herein by
reference in its entirety.
Obviously, numerous modifications and variations of the present invention are possible in light of the above teachings. It is therefore to be understood that, within the scope of the appended claims, the invention may be practiced otherwise than as specifically described herein.
21

Claims

CLAIMS:
1. A method of administering estramustine phosphate as an intravenous dose, whereby the dosage of a single infusion exceeds 1300 mg.
2. A method of administering estramustine phosphate as an intravenous dose, whereby the dosage of a single infusion exceeds 950 mg/m2.
3. The method of claims 1 or 2, wherein estramustine phosphate is administered as a single infusion on a once weekly schedule.
4. The method of claims 1 or 2, wherein estramustine phosphate is administered as a single infusion on a once every two week schedule.
5. The method of claims 1 or 2, wherein estramustine phosphate is administered as a single infusion on a once every three week schedule.
6. The method of claims 1 or 2, wherein estramustine phosphate is administered as a single infusion on a once every four week schedule.
7. The method of claims 1 or 2, wherein estramustine phosphate is administered in combination with other anti-cancer therapies.
8. The method of claim 7, wherein estramustine phosphate is administered intravenously in combination with other chemotherapeutic agents.
22
9. A method of potentiating the therapeutic benefit of a multi-drug chemotherapeutic regimen, wherein one of the drugs in the regimen comprises estramustine, by administering estramustine phosphate as an intravenous formulation.
10. The method of claim 9, wherein said intravenous formulation comprises estramustine phosphate given at high dose.
11. The method of claim 9, wherein another drug in the regimen comprises an anti-mitotic agent or anti-microtubule agent.
12. The method of claim 10, wherein the dosage of a single infusion of estramustine phosphate exceeds 1300 mg.
13. The method of claim 10, wherein the dosage of a single infusion of estramustine phosphate exceeds 950 mg/m2.
14. A method to produce prolonged elevated plasma levels of estramustine to promote synergistic interaction between estramustine and a second chemotherapeutic agent, wherein: estramustine is administered as an intravenous formulation; and estramustine is administered on the day of, or within 3 days of administration of said second chemotherapeutic agent.
15. The method of claim 14, wherein said second chemotherapeutic agent
23 comprises an anti-mitotic agent or anti-microtubule agent.
16. The method of claim 14, wherein the intravenous formulation comprises estramustine phosphate.
17. The method of claim 16, wherein the dosage of a single infusion of estramustine phosphate exceeds 1300 mg.
18. The method of claim 16, wherein the dosage of a single infusion of estramustine phosphate exceeds 950 mg/m2.
19. A method to produce elevated plasma levels of the estramustine metabolite estromustine, to promote synergistic interaction between estromustine and a second chemotherapeutic agent, wherein: estrastine is administered as an intravenous formulation; and estramustine is administered on the day of, or within 3 days of administration of said second therapeutic agent.
20. The method of claim 19, wherein said second therapeutic agent comprises an anti-mitotic agent or anti-microtubule agent.
21. The method of claim 19, wherein the intravenous formulation comprises estramustine phosphate.
24
22. The method of claim 21. wherein the dosage of a single infusion of estramustine phosphate exceeds 1300 mg.
23. The method of claim 21, wherein the dosage of a single infusion of estramustine phosphate exceeds 950 mg/m2.
24. A method according to claim 14 to potentiate therapeutic benefit.
25. A method according to claim 19 to potentiate therapeutic benefit.
26. A method to sustain plasma levels of estramustine and estromustine. wherein estramustine phosphate is administered intravenously as a single infusion at a dosage exceeding 1300 mg; optionally repeating the infusion in a serial manner.
27. A method to sustain plasma levels of estramustine and estromustine. wherein estramustine phosphate is administered intravenously as a single infusion at a dosage exceeding 950 mg/m2, optionally repeating the infusion in a serial manner.
28. A method according to claim 26. wherein therapeutic benefit is sustained.
29. A method according to claim 27. wherein therapeutic benefit is sustained.
30. A method of increasing binding saturation of estramustine to estramustine binding protein, or like-protein wherein: estramustine is administered as an intravenous formulation as estramustine phosphate at a single infusion dosage exceeding 1300 mg; and binding saturation of estramustine binding protein is thereby enhanced.
31. A method of increasing binding saturation of estramustine or its metabolites to estramustine binding protein, or like-protein wherein: estramustine is administered as an intravenous formulation as estramustine phosphate at a single infusion dosage exceeding 950 mg/m2; and binding saturation of estramustine binding protein is thereby enhanced.
32. A method of prolonging binding duration of estramustine or its metabolites to estramustine binding protein, or like-protein wherein: estramustine is administered as an intravenous formulation as estramustine phosphate at a single infusion dosage exceeding 1300 mg; and binding duration of estramustine binding protein is thereby prolonged.
33. A method of prolonging binding duration of estramustine or its metabolites to estramustine binding protein, or like-protein wherein: estramustine is administered as an intravenous formulation as estramustine phosphate at a single infusion dosage exceeding 950 mg/m2; and binding duration of estramustine binding protein is thereby prolonged.
34. The method of claim 30, wherein the method is used to treat a cancer having estramustine binding protein, or estramustine binding protein-like protein.
26
35. The method of claim 34. wherein said cancer is selected from the group consisting of prostate cancer, breast cancer, melanoma, lung cancer, pancreatic cancer, colorectal cancer, ovarian cancer, and cancers of the brain.
36. The method of claim 31. wherein the method is used to treat a cancer having estramustine binding protein, or like-protein.
37. The method of claim 36, wherein said cancer is selected from the group consisting of prostate cancer, breast cancer, melanoma, lung cancer, pancreatic cancer,
colorectal cancer, ovarian cancer, and cancers of the brain.
38. The method of claim 32, wherein the method is used to treat a cancer
having estramustine binding protein, or like-protein.
39. The method of claim 38. wherein said cancer is selected from the group
consisting of prostate cancer, breast cancer, lung cancer, pancreatic cancer, colorectal
cancer, ovarian cancer, and cancers of the brain.
40. The method of claim 33, wherein the method is used to treat a cancer having estramustine binding protein, or like-protein.
41. The method claim 40. wherein said cancer is selected from the group
consisting of prostate cancer, breast cancer, lung cancer, pancreatic cancer, colorectal cancer, ovarian cancer, melanoma, and cancers of the brain.
27
42. A method of treatment for breast cancer in which estramustine phosphate is administered intravenously.
43. A method of treatment for lung cancer in which estramustine phosphate is administered intravenously.
44. A method of treatment for pancreatic cancer in which estramustine
phosphate is administered intravenously.
45. A method of treatment for colorectal cancer in which estramustine
phosphate is administered intravenously.
46. A method of treatment for ovarian cancer in which estramustine phosphate
is administered intravenously.
47. A method of treatment for brain cancer in which estramustine phosphate is
administered intravenously.
48. The method of claim 1. wherein the infusion is given over 30 minutes to 3 hours.
49. The method of claim 2. wherein the infusion is given over 30 minutes to 3 hours.
50. The method of claim 1. wherein relief from cancer-induced urinary obstruction is achieved.
51. The method of claim 2. wherein relief from cancer-induced urinary obstruction is achieved.
52. The method of claim 1. wherein rapid relief of cancer-induced pain is achieved.
53. The method of claim 2. wherein rapid relief of cancer-induced pain is
achieved.
54. The method of claim 42. in which estramustine phosphate is administered
in combination with one or more other chemotherapeutic agents.
55. The method of claim 43. in which estramustine phosphate is administered
in combination with one or more other chemotherapeutic agents.
56. The method of claim 44. in which estramustine phosphate is administered in combination with one or more other chemotherapeutic agents.
57. The method of claim 45, in which estramustine phosphate is administered
in combination with one or more other chemotherapeutic agents.
58. The method of claim 46. in which estramustine phosphate is administered in combination with one or more other chemotherapeutic agents.
59. The method of claim 47. in which estramustine phosphate is administered in combination with one or more other chemotherapeutic agents.
60. A method of treatment for melanoma in which estramustine phosphate is administered intravenously.
61. The method of claim 60. in which estramustine phosphate is administered in combination with one or more other chemotherapeutic agents.
62. The method of claim 1 1. wherein said anti-microtubule agent is a taxane.
63. The method of claim 1 1. wherein said anti-microtubule agent is a liposome encapsulated taxane.
64. The method of claim 63. wherein said liposome encapsulated taxane is liposome encapsulated paclitaxel.
65. The method of claim 9. wherein another drug in said regimen is CPT-1 1.
66. The method of claim 9. wherein another drug in said regimen is doxorubicin.
67. The method of claim 9, wherein another drug in said regimen is etoposide.
68. The method of claim 9. wherein another drug in said regimen is navelbine.
69. The method of claim 9, wherein another drug in said regimen is vinblastine.
70. A method of potentiating the therapeutic benefit of a multi-drug chemotherapeutic regimen wherein one drug in the regimen comprises a taxane. and wherein another drug in the regimen comprises estramustine phosphate, and wherein estramustine phosphate is administered intravenously at a dosage exceeding 950 mg/m2.
71. The method of claim 15, wherein said anti-microtubule agent is a taxane.
72. The method of claim 20. wherein said anti-microtubule agent is a taxane.
73. A method of administering estramustine phosphate, wherein estramustine phosphate is first encapsulated within liposomes. and then administered intravenously.
74. A formulation of estramustine phosphate, w herein estramustine is encapsulated within liposomes.
75. A method of treating cancer wherein liposome-encapsulated estramustine phosphate is administered
76 A chemotherapeutic agent consisting of estramustine phosphate encapsulated within liposome
77 A method of treatment for prostate cancer, wherein liposome-encapsulated
-) estramustine phosphate is administered
78 A method of treatment for breast cancer, wherein liposome-encapsulated estramustine phosphate is administered.
79. A method of treatment for lung cancer, wherein liposome-encapsulated estramustine phosphate is administered
0 80 A method of treatment for pancreatic cancel .w herein liposome- encapsulated estramustine phosphate is administered
81. A method of treatment for colorectal cancer, wherein liposome- encapsulated estramustine phosphate is administered
82. A method of treatment for ovarian cancer, w herein liposome-encapsulated 5 estramustine phosphate is administered
83. A method of treatment for melanoma, wherein liposome-encapsulated estramustine phosphate is administered.
84. A formulation according to claim 74 intended for intravenous
administration.
85. A product, comprising estramustine phosphate suitable for intravenous
administration and one or more chemotherapeutic agents, as a combined preparation
for simultaneous, separate or sequential use in anticancer therapy.
86. A product according to claim 85. wherein said one or more chemotherapeutic agents are selected from the group consisting of CPT-1 1.
doxorubicin. etoposide. navelbine and a taxane derivative.
87. A product according to claim 85. wherein said estramustine phosphate
suitable for intravenous administration is used as a single dosage infusion exceeding
l jOO mg.
88. A product according to claim 85. wherein said estramustine phosphate
suitable for intravenous administration is used as a single dosage infusion exceeding
950 mg/m2.
89. A product according to anyone of claims 85 to 88 for the treatment of prostate cancer, breast cancer, melanoma, lung cancer, pancreatic cancer, colorectal
cancer, ovarian cancer or cancers of the brain.
7
90. A method for the treatment of prostate cancer, breast cancer., melanoma, lung cancer, pancreatic cancer, colorectal cancer, ovarian cancer and cancers of the brain, comprising the administration of a product according to anyone of claims from 85 to 88.
34
EP99914884A 1998-03-27 1999-03-26 Methods to potentiate intravenous estramustine phosphate Withdrawn EP1003521A4 (en)

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GB0003201D0 (en) * 2000-02-11 2000-04-05 Pharmacia & Upjohn Spa Method to potentiate the therapeutic efficacy of taxane and derivatives thereof
US6436913B1 (en) * 2000-07-25 2002-08-20 Pharmacia & Upjohn Company Use of estramustine phosphate in the treatment of bone metastasis
RU2471511C1 (en) * 2011-05-04 2013-01-10 Федеральное государственное бюджетное учреждение "Ростовский научно-исследовательский онкологический институт" Министерства здравоохранения и социального развития Российской Федерации (ФГБУ "РНИОИ" Минздравсоцразвития России) Method of treating colonic liver metastases

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US5728687A (en) * 1992-11-10 1998-03-17 Rhone-Poulenc Rorer, S.A. Antitumour compositions containing taxane derivatives

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AU3353399A (en) 1999-10-18
EA004647B1 (en) 2004-06-24
NZ501987A (en) 2002-10-25
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KR20010021656A (en) 2001-03-15
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NO20002343D0 (en) 2000-05-04
EP1003521A4 (en) 2003-07-23
ZA997821B (en) 2000-08-01
BR9906425A (en) 2000-07-11
JP2001508810A (en) 2001-07-03
HUP0200547A2 (en) 2002-07-29
NO20002343L (en) 2000-05-04
WO1999049869A1 (en) 1999-10-07
PL342969A1 (en) 2001-07-16
IL133612A0 (en) 2001-04-30
ID24504A (en) 2000-07-20

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