CN1686549A - Medicinal composition for treating high blood pressure - Google Patents

Medicinal composition for treating high blood pressure Download PDF

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CN1686549A
CN1686549A CNA2005100683199A CN200510068319A CN1686549A CN 1686549 A CN1686549 A CN 1686549A CN A2005100683199 A CNA2005100683199 A CN A2005100683199A CN 200510068319 A CN200510068319 A CN 200510068319A CN 1686549 A CN1686549 A CN 1686549A
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calcium
pharmaceutical composition
antihypertensive drug
dissimilar
calcic
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CN100389830C (en
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彭继道
刘丽笙
苏金平
杨家秀
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SHIBAI MEDICAL TECH Co Ltd GUANGZHOU CITY
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/02Inorganic compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/435Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
    • A61K31/44Non condensed pyridines; Hydrogenated derivatives thereof
    • A61K31/44221,4-Dihydropyridines, e.g. nifedipine, nicardipine
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K33/00Medicinal preparations containing inorganic active ingredients
    • A61K33/06Aluminium, calcium or magnesium; Compounds thereof, e.g. clay
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K45/00Medicinal preparations containing active ingredients not provided for in groups A61K31/00 - A61K41/00
    • A61K45/06Mixtures of active ingredients without chemical characterisation, e.g. antiphlogistics and cardiaca
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/12Antihypertensives

Abstract

A composite medicine for treating hypertension contains proportionally one or two antihypertensive medicines chosen from calcium antagon, alpha receptor blocker, beta receptor blocker, renin-angiotonin system regulator and diuretic, one Ca containing component and the farmacologically acceptable auxiliary.

Description

The hypertensive pharmaceutical composition of a kind of treatment
Technical field
The present invention relates to a kind of pharmaceutical composition, or rather, the present invention relates to the hypertensive pharmaceutical composition of a kind of treatment.
Background technology
Hypertension is that to increase with systemic arterial pressure be one of modal cardiovascular disease of main clinical manifestation, often with multiple complications such as apoplexy, myocardial infarction, heart failure, coronary heart disease, diabetes.According to China hypertension therapeutic guide regulation: the adult's systolic pressure more than 18 years old more than or equal to 140mmHg and (or) diastolic pressure is hypertension more than or equal to 90mmHg.A large amount of studies show that, it is bigger that systolic pressure increases the harm of increasing than diastolic pressure.
Investigation shows that China adult hypertension prevalence is 18.8%, estimates that national number of patients is 1.6 hundred million, increases more than 7,000 ten thousand than 1991, and rural area hypertension prevalence rises rapidly, and the town and country gap is not obvious.The hypertensive incidence trend of China has the characteristics of " three Senior Three are low ", i.e. prevalence, disability rate, mortality rate height, and awareness, the rate of taking medicine, control rate are low.Therefore how effectively controlling blood pressure has become one of focus of medical circle common concern.
Generally speaking, the hypertensive patient is than normal person's lost of life 15-20.95% hypertensive patient is an essential hypertension, and pathogenic factor is how relevant unusually with cyclical levels such as the interior feritin of patient's body, parathyroid hypertensive factor (PHF), vitamin D.
Antihypertensive drug has a lot of types at present, and medicine commonly used has calcium-channel antagonists, alpha receptor blocking agent, beta receptor blocker, renin-angiotensin system regulator (comprising tonin inhibitor and angiotensin-ii receptor blockers) and diuretic.The use of antihypertensive drug should be from low dose.The mild hypertension patient can select a kind of depressor for use, and more serious patient often needs two kinds of different types of antihypertensive drugs to unite use.But patient dependence is relatively poor, and two medicines share preferably preparation.Same hypotensor is not generally united use.Should often measure blood pressure in the medication process, observe the medication effect.If effect is bad, interchangeable another kind of antihypertensive drugs is suitably regulated consumption.Drug combination also should prevent that untoward reaction from taking place from low dose.Clinical trial confirms that will reach ideal blood pressure lowering level, 69% hypertensive patient need accept drug combination, the patient of diseases such as especially middle severe hypertension, merging target organ damage and diabetes.
1963, calcium antagonist was incorporated in the blood pressure lowering treatment first.Four during the last ten years, and calcium antagonist becomes one of main medicine of treatment hypertension.Calcium antagonist can make the open decreased number of the calcium channel of cardiac muscle and level and smooth muscle cell membrane, retardance Ca 2+Enter in the cell, thereby make smooth muscle loosening, vascular resistance descends, and brings high blood pressure down, and also target organs such as heart kidney is had protective effect simultaneously.Be particularly useful for senile hypertension, systolic hypertension, merging hyperlipemia, obesity or the hypertension of electrolyte disturbance, the hypertension of the merging heart, brain, kidney vascular complication and PA hypertension etc.Use very extensive in China.
Alpha-receptor blocker energy selective exclusion peripheral blood vessel alpha-receptor suppresses norepinephrine and discharges, and lax vascular smooth muscle reduces peripheral vascular resistance, expands small artery, brings high blood pressure down.The alpha block agent may be favourable to hyperlipidemia and impaired glucose tolerance person, can reverse left ventricular hypertrophy, improves insulin resistant, obviously improves prostate hyperplasia patient's dysuria.Pula azoles piperazine can not only bring high blood pressure down, and also reduces blood viscosity, keeps the normal heart, brain, renal blood flow supply, does not influence glomerular filtration, and is particularly effective to the hyperpietic with renal insufficiency.
The beta receptor blocker is to be widely used in the hypertensive line medicine of treatment, is applicable to sympathetic hyperfunction or the hyperpietic of angina pectoris, tachy-arrhythmia is arranged.Such medicine retardance beta receptor weakens myocardial contraction, reduces cardiac output, reduces myocardial oxygen consumption, suppresses the secretion of feritin, the purpose that reaches decreased heart rate and bring high blood pressure down.The beta receptor blocker is to hypertensive patients coronary heart disease, particularly the patient behind acute coronary syndrome and the myocardial infarction is very effective, " optimal drug " that is considered to the coronary heart disease secondary prevention, beta receptor blocker still are the strong indication of hypertensive patients heart failure, diabetes.Beta-blocker and diuretic, calcium antagonist share good hypotensive effect.
Renin-angiotensin system (RAS) regulator comprises tonin inhibitor (ACE I) and angiotensin-ii receptor blockers.The application of ACE I is the much progress on the antihypertensive drug therapeutics.Such medicine can suppress tonin (ACE I) activity, and the generation minimizing of Angiotensin II (Ang II) and the degraded of Kallidin I are reduced, and blood vessel dilating brings high blood pressure down.Such medicine not only has good antihypertensive effect, and hypertensive complications and some concomitant diseases are also had desirable influence, is available as the choice drug with the hyperpietic of diabetes, left ventricular hypertrophy, left heart function obstacle and acute myocardial infarction.Such medicine has slight retention K +Effect, the patient that hyperkalemia is arranged is noticed particularly vasodilation causes the patient, and intractable cough takes place is the rare and serious adverse effects of this medicine.Ang II is the main active substances of RAS, is one of hormone the strongest in the known endogenous material that boosts and important and intensive endogenous vasoconstrictive factor.The angiotensin-ii receptor blockers great advantage is the strong point that has kept the angiotensin-convertion enzyme inhibitor effect, and has overcome its most of weakness, completely without the untoward reaction that causes paroxysmal spasmodic cough.
Change Na in the body with medicine +Balance becomes one of hypertensive main method of treatment.The diuretic blood pressure lowering starts from 1948, diuretic blood pressure lowering by reducing extracellular fluid volume and cardiac output; Vascular resistance descends to some extent after the long term administration.According to the result of extensive clinical trial in the world, prove that the diuretic antihypertensive effect is sure, and can strengthen the effect of other depressor.Uncomplicated hypertensive patient all advises in the several hypertension treatment principle of America and Europe committee, is choice drug with the diuretic.The diuretic especially hyperpietic's effect to old people, obesity is more obvious.
Novel antihypertensive also comprises endothelin-receptor antagonists, neuropeptide tyrosine inhibitor, atrial natriuretic peptide and endopeptidase inhibitor; Imidazoles woods receptor agonist, 5-hydroxytryptamine receptor antagonist, K +Channel opener, calcitonin-gene-related peptide (CGRP) etc.But clinical practice is also few at home for these new drugs at present.
Disclose the hypertensive pharmaceutical composition of a kind of treatment among the CN1562369 A, wherein contained calcium ion antagonist, diuretic, aldosterone antagonists of certain weight ratio etc.
Antihypertensive, by general recommended dose, typical situation and placebo, mean blood pressure is 160/95mmHg, then single therapy reduces systolic pressure 7-15mmHg and diastolic pressure 4-10mmHg usually; Unite other antihypertensive drug, can make blood pressure drops 8-15%, be i.e. systolic pressure decline 12-24mmHg and diastolic pressure decline 8-12mmHg.
Usually medicine therapy is generally by three kinds of approach shown in Figure 8.
Approach 1 shows main paathogenic factor thereby minority target organ generation effect is caused the movable pathological symptom that occurs of cell pathology.Yet other organ or cell are not affected in the body, and cellular activity is normal.Different responses is the crucial starting point of medicine design and development to " pathology defective " tissue to paathogenic factor with " normally " tissue.
The present situation that the most Western medicine of approach 2 representatives are cured the disease, this type of medicine plays a role at one or several pathological tissue.Most applications lower body biochemical or physically differently all set forth clearlyer, the medicine of design is by changing one or certain several pathological tissues to improve clinical symptoms.In order to make destination organization or tissue conditions obtain substantial control, need take a large amount of medicines.These medicines have very strong pharmacologically active, also can exert an influence to other normal structure simultaneously, therefore have side effects.
Approach 3 is represented a kind of comparatively ideal state of Drug therapy.If main paathogenic factor is known, can suppress paathogenic factor or directly produce physiologically active by the design medicine, so the pathological tissues recovery is normal, thereby disease symptoms is controlled.Medicine suppresses paathogenic factor to health tissues generation effect, and normal health is organized the influence that is not subjected to paathogenic factor, thereby side effects of pharmaceutical drugs are less.In theory, this is a very ideal approach of new drug development.Yet, there is following problem: at first, most of disease, its main paathogenic factor is not quite clear; Secondly, the numerous diseases complication is more; The 3rd, even the cause of disease knows that it almost is impossible that a kind of chemical constituent can suppress all causes of disease.
Antihypertensive drug obtains very big development over 50 years.But hypertension is as the uncertain disease of a kind of cause of disease, and the effect cure rate of one or more that medicine produces at a kind of cause of disease or the mechanism of action is lower, and the cure rate of common a kind of medicine is about 40-50%, and prognosis is relatively poor.In recent years, though the depressor of much new good effect few side effects is arranged, the controlling blood pressure rate also can only reach 50-60%.Therefore, a kind of new treatment pattern is applied to clinical gradually, and the compound hypertension medicine preparation is internationally recognized a kind of orientation treatment.Inventor's years of researches prove: the hyperpietic near 70% needs drug combination.Because the compound antihypertensive drug prescription is followed the principle that different mechanism of action medicines carry out proportioning usually, therefore show as the advantage that increases curative effect or reduce side effect, obtain better controlling of blood pressure effect, thereby finished the present invention.
Summary of the invention
One object of the present invention is to provide a kind of hypertensive pharmaceutical composition that is used for the treatment of.
Another object of the present invention is to provide the application of said composition in the hypertensive medicine of preparation treatment.
The hypertensive pharmaceutical composition of a kind of treatment provided by the invention, it is characterized in that said composition comprise a kind of or two kinds of dissimilar antihypertensive drug and a kind of calcic component and pharmacy on acceptable auxiliary.
Described antihypertensive drug is selected from calcium antagonist, alpha receptor blocking agent, beta receptor blocker, renin-angiotensin system regulator and diuretic.
Described calcium antagonist is selected from nifedipine, amlodipine, felodipine, lacidipine, nitrendipine, nicardipine, nimodipine, nisoldipine, Buddhist nun's dagger-axe Horizon, isradipine, verapamil and diltiazem.This calcium antagonist is preferably nifedipine or nitrendipine.
Described alpha receptor blocking agent is selected from pula azoles piperazine (prazosin), terazosin, doxazosin, trimazosin, phenoxybenzamine and phentolamine.This alpha receptor blocking agent is preferably pula azoles piperazine.
Described beta receptor blocker is selected from nadolol, acebutolol, labetalol, metoprolol, bisoprolol, esmolol, Propranolol (propranolol), atenolol (atenolol), carvedilol.This beta receptor blocker is preferably atenolol.
Described renin-angiotensin system regulator is selected from captopril (captopril), enalapril, benazepril, fosinopril (MENGNUO), lisinopril, quinapril, ramipril, perindopril, cilazapril, losartan, valsartan, telmisartan, irbesartan, Candesartan.This renin-angiotensin system regulator is preferably enalapril.
Described diuretic is selected from furosemide (FRUSEMIDE), acidum ethacrynicum, bumetanide, Torasemide, hydrochlorothiazide (hydrochlorothiazide), chlorothiazide, Indapamide, chlortalidone, metolazone, quinethazone, triamterene, amiloride, spironolactone, acetazolamide.This diuretic is preferably furosemide or hydrochlorothiazide.
The calcic component refer to can for human body take various calcareous, it is to be selected from shell, Os Draconis, calcium chloride, calcium carbonate, calcium phosphate, calcium citrate, calcium lactate, calcium gluconate or the l threonic acid one or more, and wherein shell comprises Concha Margaritifera, Concha Ostreae, Concha Haliotidis or its activation product calcium oxide.This calcic component is preferably calcium gluconate and/or calcium citrate.
If this pharmaceutical composition comprises a kind of or two kinds of dissimilar antihypertensive drug and a kind of calcic component, the proportioning of described two types of antihypertensive drug and calcic component is 0-50: 0-50: 10-2000 by weight, be preferably 0-30: 0-30: 15-1000,0-20: 0-20: 20-500 more preferably, the content of wherein dissimilar antihypertensive drug is not 0 simultaneously, and the calcic component is with Ca 2+Meter.
If this pharmaceutical composition comprises one type antihypertensive drug and a kind of calcic component, then this antihypertensive drug does not comprise diuretic, the proportioning of this antihypertensive drug and calcic component is 1 by weight: 10-2000, be preferably 1: 15-1000, more preferably 1: 20-500, wherein the calcic component is with Ca 2+Meter.
The present invention treats and contains an amount of adjuvant in the hypertensive compositions, and wherein adjuvant is sucrose, lactose, galactose, maltose, mannitol, sorbitol, starch, corn starch, dextrin.
Can also add acceptable disintegrating agent, lubricant, coloring agent, correctives in an amount of pharmacy in the present composition.
The present composition can be made said dosage form on any pharmaceutics, is good with tablet, the capsule of oral administration.
The invention still further relates to the application of said composition in the hypertensive medicine of preparation treatment.
It is reported that the absorption of heavy dose of calcium can produce pressure reduction effect.Yet this discovery can not successfully repeat in whole research process.In addition, this type of pressure reduction effect that dietary calcium produces is quite clear in low renin level, the responsive patient of salt, and calcium antagonist has curative effect preferably to this class patient.This is a very absurd conclusion seemingly.A lot of experts of this research field attempt to find a proper explanations, all do not achieve success.
Through studying for a long period of time and a large amount of test, compositions of the present invention provides solution for the problems referred to above.
The present invention adopts spontaneous hypertensive rat (SHR) to test the pressure reduction effect of calcium and calcium antagonist drug combination, and clinical patient has been carried out the observation of curative effect of calcium+calcium antagonist and calcium+alpha receptor blocking agent drug combination.The result is as follows:
1. calcium has strengthened the hypotensive effect of low dosage calcium antagonist or alpha receptor blocking agent;
2. calcium has improved prognosis effect and effective percentage, but dependent interaction is not obvious in taking calcium antagonist or alpha receptor blocking agent separately.
Core of the present invention is the special role of calcium in hypertension therapeutic.Calcium can suppress the feritin level, has the parathyroid gland activity, reduces the cyclical level and 1 of parathyroid hypertensive factor (PHF) in patient's body, 25-two-hydroxyl-vitamin D 3Physiologically active; Antihypertensive can suppress hypertensive symptom, alleviates the infringement to target organ.Thereby calcium can strengthen the effect that brings high blood pressure down of the antihypertensive of low dosage, realizes target shown in Figure 9.
Description of drawings
Fig. 1 represents that calcium strengthens the experimentation of the hypotensive activity of nifedipine.
Fig. 2 represents that calcium strengthens the experimentation of the hypotensive activity of furosemide.
Fig. 3 represents that calcium strengthens the experimentation of the hypotensive activity of hydrochlorothiazide.
Fig. 4 represents that calcium adds the test data statistical table of nitrendipine to the influence of human body systolic pressure (SBP).
Fig. 5 represents that calcium adds the test data statistical table of pula azoles piperazine to the influence of human body systolic pressure (SBP).
Fig. 6 represents that calcium adds the test data statistical table of furosemide to the influence of human body systolic pressure (SBP).
Fig. 7 represents that calcium adds the test data statistical table of hydrochlorothiazide to the influence of human body systolic pressure (SBP).
Fig. 8 represents three kinds of approach of common medicine therapy in the prior art.
Fig. 9 represents the target that the special role of calcium in hypertension therapeutic promptly realizes.
The specific embodiment
The following examples are only in order to further specify the present invention, rather than limit the scope of the invention.
At first adopt following method and proportioning that pharmaceutical composition of the present invention is made tablet or capsule respectively:
Preparation method 1: with the fine powder and the appropriate amount of auxiliary materials mix homogeneously of effective ingredient in this pharmaceutical composition, compressing dry granulation or pelletizing press sheet according to a conventional method.But tablet sugar coating, film-coat or coating not, the heavy 100-1000mg of sheet;
Preparation method 2: with the fine powder and the appropriate amount of auxiliary materials mix homogeneously of effective ingredient in this pharmaceutical composition, wet granulation or with the direct filled capsules of powder according to a conventional method.The heavy 100-1000mg of capsule.
Embodiment 1:
Nifedipine 5.0mg, calcium citrate 1000mg, starch 180mg, sucrose 15mg.
Embodiment 2:
Nitrendipine 5.0mg, calcium gluconate 2000mg, starch 380mg, dextrin 15mg.
Embodiment 3:
Pula azoles piperazine 0.5mg, calcium gluconate 2000mg, corn starch 380mg, dextrin 19.5mg.
Embodiment 4:
Atenolol 6.25mg, calcium gluconate 2000mg, starch 380mg, dextrin 13.75mg.
Embodiment 5:
Enalapril 2.5mg, calcium citrate 1000mg, starch 190mg, dextrin 7.5mg.
Embodiment 6:
Pula azoles piperazine 0.5mg, nitrendipine 5.0mg, calcium gluconate 2000mg, starch 380mg, dextrin 14.5mg.
Embodiment 7:
Atenolol 5.0mg, nitrendipine 5.0mg, calcium citrate 1000mg, starch 190mg, dextrin 10.0mg.
Embodiment 8:
Nitrendipine 4.0mg, enalapril 2.5mg, calcium gluconate 2000mg, starch 380mg, dextrin 13.5mg.
Embodiment 9:
Hydrochlorothiazide 5.0mg, enalapril 2.5mg, calcium gluconate 2000mg, starch 380mg, dextrin 12.5mg.
Embodiment 10:
Nitrendipine 4.0mg, furosemide 5.0mg, calcium gluconate 2000mg, starch 380mg, dextrin 11.0mg.
What deserves to be mentioned is that the consumption of calcium is according to Ca 2+Ratio shared in the calcic component adds.
W Ca2+=W HF*(M ca2+/M HF*100%)
W Ca2+The consumption of expression calcium;
W HFThe consumption of calcic component in the expression prescription;
M Ca2+/ M HF* 100% represents the percentage composition of calcium in the calcic component.
To further specify the beneficial effect of pharmaceutical composition of the present invention in the hypertensive medicinal application of preparation treatment by animal experiment and anthroposcopy below.Accompanying drawing 1 is based on the zoopery result of nifedipine+calcium group; Accompanying drawing 2 is based on the zoopery result of furosemide+calcium group; Accompanying drawing 3 is based on the zoopery result of hydrochlorothiazide+calcium group; Accompanying drawing 4 is based on the anthroposcopy effect of nitrendipine+calcium group; Accompanying drawing 5 is based on the anthroposcopy effect of pula azoles piperazine+calcium group; Accompanying drawing 6 is based on the anthroposcopy effect of furosemide+calcium group; Accompanying drawing 7 is based on the anthroposcopy effect of hydrochlorothiazide+calcium group.The compositions that experiment showed, two kinds of dissimilar antihypertensive+calcium can obtain useful effect equally.
Animal experiment
SHR is that a kind of optimum with genetic background is studied human hyperpietic animal model.
Get 8 all male SHR rats in age (available from State-Run Yangming University's Experimental Animal Center, the Taibei, Taiwan), under laboratory environment, raised for two weeks, stroke every day then the training continuous two weeks more than, and under wide-awake state, put into the tail vein pressure measuring device [I ' hysiograph (Model:DMP-4B) Narco Bio-systems, Inc.Houston, TX, USA], measure the afterbody blood pressure by the folder tail, measure blood pressure weekly three times, relatively stable up to pressure value, can test.
The drop test of nifedipine
During test, SHR is divided into 3 groups at random.Get a certain amount of tested sample and distilled water according to the body weight of rat.Nifedipine group is 10mg/kg, qd; Nifedipine+calcium group is nifedipine 10mg/kg, qd+ Concha Margaritifera superfine powder 500mg/kg, qd; Matched group is distilled water 7.5ml/kg, qd.Give the rat medicine feed by a stomach tube under waking state, blood pressure is measured weekly three times.Observed 1 month, the blood pressure that administration is two groups all significantly decreases, and adds calcium and does not add the two drop-out value of blood pressure of calcium and do not have evident difference.Adjust dosage: Nifedipine group is 3.33mg/kg, qd; Nifedipine+calcium group is the flat 3.33mg/kg of nitre benzene, qd+ Concha Margaritifera superfine powder 500mg/kg, qd; Matched group is distilled water 7.5ml/kg, and qd continue to observe one month, and adding the calcium group, not add the blood pressure drops of calcium group obvious, and the two reaches 15mmHg, the result as shown in Figure 1, the result shows: add calcium and can strengthen hypotensive activity than the nifedipine under the low dosage.
The drop test of furosemide:
During test, SHR is divided into 3 groups at random.Get a certain amount of tested sample and distilled water according to the body weight of rat.The furosemide group is 35mg/kg/d; Furosemide+calcium group is furosemide 35mg/kg/d+ Concha Margaritifera superfine powder 2000mg/kg/d; Matched group is distilled water 7.5ml/kg/d.Give the rat medicine feed by a stomach tube under waking state, blood pressure is measured weekly three times or is measured according to practical situation, reduces to certain level when no longer descending when blood pressure, stops administration and further the recovery situation of blood pressure is observed, and collects pressure value and calculates.Observed for two weeks, the result shows: independent furosemide does not have tangible hypotensive effect (blood pressure drops 3-6mmHg) during low dosage, adds the hypotensive activity (blood pressure drops 10-15mmHg) that calcium can strengthen the furosemide of same dose, and the result as shown in Figure 2.The result proves that calcium can strengthen the hypotensive effect of the furosemide of low dosage.
The drop test of hydrochlorothiazide:
During test, SHR is divided into 3 groups at random, and gets tested sample and distilled water according to the body weight of rat, and during on-test, the hydrochlorothiazide group is 4mg/kg.qd; Hydrochlorothiazide+calcium group is hydrochlorothiazide 4mg/kg.qd+ Concha Margaritifera superfine powder 500mg/kg.qd; Matched group is distilled water 7.5ml/kg.qd, under waking state, give the rat medicine feed by stomach tube, blood pressure is measured weekly three times or is measured according to practical situation, when blood pressure is reduced to certain level when no longer descending, stop administration and further the recovery situation of blood pressure is observed collection pressure value and calculating.Observed two months, the blood pressure that administration is two groups all significantly decreases, and adds calcium and does not add the two drop-out value of blood pressure of calcium and do not have evident difference.Adjust dosage: the hydrochlorothiazide group is 1.33mg/kg.qd; Hydrochlorothiazide+calcium group is hydrochlorothiazide 1.33mg/kg.qd+ Concha Margaritifera superfine powder 500mg/kg.qd; Matched group is distilled water 7.5ml/kg.qd, continue to observe one and a half months, adding the calcium group, not add the blood pressure drops of calcium group obvious, and the two differs 5-10mmHg, the result as shown in Figure 3, the result shows: add calcium and can strengthen hypotensive activity than the hydrochlorothiazide under the low dosage.
The human body medication is observed:
Choose that community clinic is light, the moderate blood pressure is at the primary hypertension patient of 140-180/90-109mmHg, male or female, the age is more than 35 years old.Secondary hypertension, the depletion of hypertensive patients cardiorenal function, serum creatinine 〉=3mg/dl, to ACEI allergies, anemia of pregnant woman are arranged and the patient that can not cooperate with doctor selected, dailyly take the selected of calcium tablet.Emptied for two weeks before on-test, around successive administration is observed.Specific drug is oral once a day, checks blood pressure and heart rate during the treatment weekly, writes down three right upper arm seat blood pressures and heart rate, and inquiry adverse reactions of patients situation.
Nitrendipine+calcium is to the influence of human blood-pressure
Fig. 4: calcium strengthens the anthroposcopy research of the hypotensive activity of nitrendipine.Patient is divided into two groups at random, and A1 of observation group and control group A 2 respectively are 25 patients.A1 group dosage is nitrendipine 5mg/d+ calcium gluconate 2000mg/d (being equivalent to calcium 178.6mg/d), and A2 group nitrendipine is 5mg/d.Fig. 4 is the statistical data of medicine to the influence of patient's systolic pressure (SBP).Statistical result shows: nitrendipine is when low dosage, and matched group and observation group compare, and the systolic pressure of observation group reduces obviously than the systolic pressure of matched group.According to the standard of " Chinese hypertension prevention and control guide ", reach through treating the after-contraction pressure</=140mmHg person is normal (being produce effects); Reach</=160mmHg person is control (promptly effective).Per os took medicine for 2 weeks afterwards in this experiment: observation group's obvious effective rate is 80%, and effective percentage is 20%; And the matched group obvious effective rate is 64%, and effective percentage is 36%.
Pula azoles piperazine+calcium is to the influence of human blood-pressure
Fig. 5: calcium strengthens the anthroposcopy research of the hypotensive activity of pula azoles piperazine.Patient is divided into two groups at random, and D1 of observation group and matched group D2 respectively are 25 patients.D1 group dosage is pula azoles piperazine 0.5mg/d+ calcium gluconate 2000mg/d (being equivalent to calcium 178.6mg/d), and D2 group pula azoles piperazine is 0.5mg/d.Fig. 5 is the statistical data of medicine to the influence of patient's systolic pressure (SBP).Statistical result shows that matched group and observation group compare, and the systolic pressure of observation group is obvious than the systolic pressure reduction effect of matched group.According to the standard of " Chinese hypertension prevention and control guide ", reach through treating the after-contraction pressure</=140mmHg person is normal (being produce effects); Reach</=160mmHg person is control (promptly effective).Per os took medicine for 2 weeks afterwards in this experiment: observation group's obvious effective rate is 88%, and effective percentage is 8%, and inefficiency is 4%; And the matched group obvious effective rate is 64%, and effective percentage is 32%, and inefficiency is 4%.
Furosemide+calcium is to the influence of human blood-pressure
Fig. 6: strengthen the anthroposcopy research of the hypotensive activity of furosemide for calcium.Patient is divided into two groups at random, and C1 of observation group and matched group C2 respectively are 25 patients.C1 group dosage is furosemide 5mg/d+ calcium gluconate 2000mg/d (being equivalent to calcium 178.6mg/d), and C2 group furosemide is 5mg/d.Fig. 6 is the statistical data of medicine to the influence of patient's systolic pressure (SBP).Statistical result shows: furosemide is when low dosage, and matched group and observation group compare, and the systolic pressure of observation group reduces obviously than the systolic pressure of matched group.According to the standard of " Chinese hypertension prevention and control guide ", reach through treating the after-contraction pressure</=140mmHg person is normal (being produce effects); Reach</=160mmHg person is control (promptly effective).Per os took medicine for 2 weeks afterwards in this experiment: observation group's obvious effective rate is 96%, and effective percentage is 4%; And the matched group obvious effective rate is 48%, and effective percentage is 44%, and inefficiency is 8%.
Hydrochlorothiazide+calcium is to the influence of human blood-pressure
Fig. 7: calcium strengthens the anthroposcopy research of the hypotensive activity of hydrochlorothiazide.Patient is divided into two groups at random, and F1 of observation group and matched group F2 respectively are 25 patients.F1 group dosage is hydrochlorothiazide 6.25mg/d+ calcium gluconate 2000mg/d (being equivalent to calcium 178.6mg/d), and F2 group hydrochlorothiazide is 6.25mg/d.Fig. 7 is the statistical data of medicine to the influence of patient's systolic pressure (SBP).Statistical result shows that matched group and observation group compare, and the systolic pressure of observation group is obvious than the systolic pressure reduction effect of matched group.According to the standard of " Chinese hypertension prevention and control guide ", reach through treating the after-contraction pressure</=140mmHg person is normal (being produce effects); Reach</=160mmHg person is control (promptly effective).Per os took medicine for 2 weeks afterwards in this experiment: observation group's obvious effective rate is 92%, and effective percentage is 8%; And the matched group obvious effective rate is 72%, and effective percentage is 24%, and inefficiency is 4%.
The present composition and independent diuretic and novel antihypertensive drugs are compared as follows table:
Diuretic Novel antihypertensive drugs Product of the present invention
Curative effect Low High High
Effective percentage (%) patent side effect investment Low nothing is obviously low Low high in the low protection period Height can be applied for low
Though the present invention has been described in detail and describes, those skilled in the art are to be understood that: under the prerequisite of not leaving the described spirit and scope of claim of the present invention, can make various changes to form of the present invention and details.

Claims (10)

1. hypertensive pharmaceutical composition of treatment, it is characterized in that said composition comprise a kind of or two kinds of dissimilar antihypertensive drug and a kind of calcic component and pharmacy on acceptable auxiliary.
2. the described pharmaceutical composition of claim 1, it is characterized in that described antihypertensive drug is selected from calcium antagonist, alpha receptor blocking agent, beta receptor blocker, renin-angiotensin system regulator and diuretic, the calcic component is various calcareous for what can supply human body to take, it is to be selected from shell, Os Draconis, calcium chloride, calcium carbonate, calcium phosphate, calcium citrate, calcium lactate, calcium gluconate or the l threonic acid one or more, and wherein shell comprises Concha Margaritifera, Concha Ostreae, Concha Haliotidis or its activation product calcium oxide.
3. the described pharmaceutical composition of claim 2, it is characterized in that described calcium antagonist is selected from nifedipine, amlodipine, felodipine, lacidipine, nitrendipine, nicardipine, nimodipine, nisoldipine, Buddhist nun's dagger-axe Horizon, isradipine, verapamil and diltiazem, described alpha receptor blocking agent is selected from pula azoles piperazine, terazosin, doxazosin, trimazosin, phenoxybenzamine and phentolamine, described beta receptor blocker is selected from nadolol, acebutolol, labetalol, metoprolol, bisoprolol, esmolol, Propranolol, atenolol and carvedilol, described renin-angiotensin system regulator is selected from captopril, enalapril, benazepril, fosinopril, lisinopril, quinapril, ramipril, perindopril, cilazapril, losartan, valsartan, telmisartan, irbesartan, Candesartan, described diuretic is selected from furosemide, acidum ethacrynicum, bumetanide, Torasemide, hydrochlorothiazide, chlorothiazide, Indapamide, chlortalidone, metolazone, quinethazone, triamterene, amiloride, spironolactone, acetazolamide.
4. the described pharmaceutical composition of claim 3, it is characterized in that described calcium antagonist is nifedipine or nitrendipine, described alpha receptor blocking agent is a pula azoles piperazine, described beta receptor blocker is an atenolol, described renin-angiotensin system regulator is an enalapril, and described diuretic is furosemide or hydrochlorothiazide.
5. the described pharmaceutical composition of claim 2 is characterized in that described calcic component is calcium gluconate and/or calcium citrate.
6. any described pharmaceutical composition of claim 1-5, it is characterized in that said composition comprises a kind of or two kinds of dissimilar antihypertensive drug and a kind of calcic component, the proportioning of described two types of antihypertensive drug and calcic component is 0-50: 0-50: 10-2000 by weight, the content of dissimilar antihypertensive drug is not 0 simultaneously, and wherein the calcic component is with Ca 2+Meter.
7. any described pharmaceutical composition of claim 1-5, it is characterized in that said composition comprises a kind of or two kinds of dissimilar antihypertensive drug and a kind of calcic component, the proportioning of described two types of antihypertensive drug and calcic component is 0-30: 0-30: 15-1000 by weight, the content of wherein dissimilar antihypertensive drug is not 0 simultaneously, and wherein the calcic component is with Ca 2+Meter.
8, any described pharmaceutical composition of claim 1-5, it is characterized in that said composition comprises a kind of or two kinds of dissimilar antihypertensive drug and a kind of calcic component, the proportioning of described two types of antihypertensive drug and calcic component is 0-20: 0-20: 20-500 by weight, the content of wherein dissimilar antihypertensive drug is not 0 simultaneously, and wherein the calcic component is with Ca 2+Meter.
9, any described pharmaceutical composition of claim 1-5 is characterized in that said composition is the tablet or the capsule of oral administration.
10, the application of any described pharmaceutical composition of claim 1-5 in the hypertensive medicine of preparation treatment.
CNB2005100683199A 2005-05-08 2005-05-08 Medicinal composition for treating high blood pressure Expired - Fee Related CN100389830C (en)

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CN101478956B (en) * 2006-06-27 2013-03-20 诺瓦提斯公司 Solid dosage forms of valsartan, amlodipine and hydrochlorothiazide and method of making the same
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CN101478956B (en) * 2006-06-27 2013-03-20 诺瓦提斯公司 Solid dosage forms of valsartan, amlodipine and hydrochlorothiazide and method of making the same
CN103169711A (en) * 2006-06-27 2013-06-26 诺瓦提斯公司 Solid dosage forms of valsartan, amlodipine and hydrochlorothiazide and method of making same
CN102058872B (en) * 2009-11-17 2013-12-25 北京万全阳光医学技术有限公司 Medicinal composition containing Lysinopril and amlodipine besilate and preparation method thereof
CN102462844A (en) * 2010-11-05 2012-05-23 四川滇虹医药开发有限公司 Tilisolol pharmaceutical composition and its preparation method
CN104758290A (en) * 2015-03-09 2015-07-08 西安力邦肇新生物科技有限公司 A compound antihypertensive composition and applications thereof
CN104758932A (en) * 2015-03-09 2015-07-08 西安汉丰药业有限责任公司 A metolazone composite preparation and applications thereof
CN104758932B (en) * 2015-03-09 2018-07-31 西安汉丰药业有限责任公司 A kind of medetofazone compound preparation and its application
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CN114569600B (en) * 2022-04-19 2023-08-08 佳木斯大学 Pharmaceutical composition for preventing and treating hypertension and application thereof

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