Pharmaceutical composition for suppression of the expression of ATP citrate lyase and use thereof

Information

  • Patent Application
  • 20050096367
  • Publication Number
    20050096367
  • Date Filed
    November 29, 2004
    20 years ago
  • Date Published
    May 05, 2005
    19 years ago
Abstract
The present invention provides a pharmaceutical composition for suppression of the expression of ATP citrate lyase, which contains a compound that suppresses the expression of ATP citrate lyase by the in vivo administration. The compounds suppress the expression of ATP citrate lyase by the in vivo administration include insulin secretagogues such as nateglinide. This pharmaceutical composition is effective in preventing, improving and treating metabolic syndrome, in particular, liver disorders related to abnormal lipid metabolism such as fatty liver and NASH.
Description
BACKGROUND OF THE INVENTION

The present invention relates to a pharmaceutical composition for suppression of the expression of ATP citrate lyase, in particular, a pharmaceutical composition for suppression of the expression of ATP citrate lyase containing nateglinide or a pharmaceutical composition for preventing, improving and/or treating metabolic syndrome, fatty liver, NASH and liver disorders.


As the dietary habits have been westernized recently, patients with metabolic syndrome having symptoms of a severe insulin resistance, obesity, hypertension, hyperlipemia and hyperglycemia and also patients with syndrome X, insulin resistant syndrome and multiple risk factor syndrome are increasing in number. In particular, patients having symptoms related to abnormal lipid metabolism such as obesity and fatty liver have a high risk of suffering from non-alcoholic steato-hepatitis (NASH). Under these circumstances, it is an important problem to develop a method for preventing, improving and treating these hepatic diseases (Gastroenterology, 121:710 (2001)).


As medicines for improving abnormal lipid metabolism, there have been known statin(s) which are inhibitors from HMGCoA, i. e. an enzyme relating to cholesterol synthesis, fibrates which activate transcription factor PPARα and glitazones which activate PPAR γ. Although these medicines were reported to improve hypercholesterolemia, hypertriglyceridemia and hyperglycemia with insulin resistance, they do not improve the whole abnormal lipid metabolism accompanying metabolic syndrome. Further, although it was reported that some of the above-described medicines or metformin used as a hypoglycemic agent is also effective on NASH (Hepatology, 33:1338 (2001)), the effect thereof is not yet satisfactory.


ATP citrate lyase (hereinafter referred to as “ACL”) is positioned at the uppermost part of the stream of the fat synthesis pathway. ACL is an enzyme which forms acetyl CoA used as a starting material in the synthesis of lipids in the cells from citric acid which is an intermediate in the glycolytic pathway. As inhibitors for this enzyme, there have been reported compounds from microorganisms (A. Antibiot., 50:729 (1997), Japanese Patent Kokai No. JP 2001-261682) and citric acid analogs (Eur. J. Biochem., 202:889 (1991), J. Med. Chem., 35:4875 (1992) and J. Med. Chem., 38, 537 (1995)). It was reported that in those inhibitors, gamma-lactone prodrugs of (3R,5S)-omega-substituted-3-carboxy-3,5-dihydroxyalkanoic acids inhibit the synthesis of cholesterol and fatty acids from liver cell line HepG2 and that blood cholesterol and triglyceride level of rats or dogs can be lowered by the in vivo administration of the prodrugs (J. Med. Chem., 41:3582 (1998)). A therapeutic agent for hyperlipemia which contains the prodrug and a method for treating hyperlipemia with this agent were applied for patent (WO 93/22304). However, compounds capable of controlling the ACL expression level per se by the in vivo administration thereof have not yet been known. The expression of ACL is physiologically elevated when carbohydrates are taken after the fasting. It is known that the expression is constitutively elevated in animals with metabolic syndrome (J. Biol. Chem., 274:30028 (1999), J. Biol. Chem., 274:35832 (1999) and J. Biol. Chem., 276:38337 (2001)). However, it has not yet been reported to find a compound which suppresses the elevated ACL expression and to use this compound for the prevention, improvement and treatment of metabolic syndrome, in particular, obesity and liver diseases such as fatty liver and NASH.


On the other hand, nateglinide is a compound capable of reacting on pancreatic β cells to rapidly stimulate the insulin secretion (Br. J. Pharmacol., 120:137 (1997)). The use of nateglinide alone as a hypoglycemic agent (Japanese Patent Kokoku No. Hei 4-15221) or as a remedy for diabetic complication and neuropathy (WO 0168136) were reported. It was also reported that a combination of nateglinide with another medicine is usable for the prevention, inhibition of advance and treatment of the following diseases and conditions associated with abnormal metabolism, particularly diabetes mellitus: hyperglycemia, hyperinsulinemia, hyperlipemia, insulin resistance, impaired glucose metabolism, obesity, diabetic retinopathy, macular degeneration, cataracts, diabetic nephropathy, glomerulosclerosis, diabetic neuropathy, erectile dysfunction, premenstrual syndrome, vascular restenosis, ulcerative colitis, coronary heart disease, hypertension, angina, myocardial infarction, stroke, disorders of skin and connective tissue, foot ulcerations, metabolic acidosis, arthritis, osteoporosis and impaired glucose tolerance (WO 01/21159, WO 01/26639). However, the effects of nateglinide on the expression of ACL have not been reported. It was also reported that insulin stimulates the expression of ACL to the contrary (Yonsei. Med. J., 35:25 (1994)). Thus, there has never been reported that nateglinide suppresses the expression of ACL specific to the metabolic syndrome and that nateglinide is effective on hepatic diseases related to metabolic syndrome, particularly abnormal lipid metabolism.


On the other hand, although many cases of clinical results with insulin secretagogue have been reported, the effects thereof on liver diseases and liver functions are yet unknown. For example, it was reported that no significant alterations in liver function were observed after 30 days' administration of nateglinide (Drugs R&D; 2(2):123 (1999)). However, in this experiment, the patients did not suffer from liver diseases. It was reported that hepatic cirrhosis had no significant effect on the pharmacokinetics of nateglinide (J. Clin. Pharmacol., 40:634 (2000), Drugs, 60(3):607 (2000)) and that nateglinide must be carefully given to patients with chronic liver diseases because the total exposure was increased by 30% in subjects with mild hepatic impairment (Am J Health-Syst Pharm, 58, 285 (2001)). However, these reports are not for describing the effects of the medicine on the liver diseases. Incremental liver function test values (GOT, GPT), that were considered to be possibly related to the study drug, have been reported infrequently (Diabetes Care 23; 202 (2000), Diabetes Care 24; 73 (2001), Ann. Pharmacother. 35:1426 (2001)). However, also these reports only relate to the safety of the medicines and the effects of the medicines on liver diseases are not described therein. It was also reported that hepatic enzyme levels is increased with the combination of nateglinide with thiazolidinedion (troglitazone) (Am J Health-Syst Pharm, 58 1200 (2001), Diabetes Care 25; 1529 (2002)). However, it is described therein that this increase is due to the treatment with troglitazone. Namely, it has never been reported at all that an insulin secretagogue such as nateglinide improves liver diseases or liver function (hepatic enzyme levels such as GOT or GPT).


DISCLOSURE OF THE INVENTION

An object of the present invention is to provide a pharmaceutical composition for suppression of the expression of ACL.


Another object of the present invention is to provide a composition for preventing, improving and treating metabolic syndrome.


Another object of the present invention is to provide a composition for preventing, improving and treating fatty liver.


Another object of the present invention is to provide a composition for preventing, improving and treating NASH.


Another object of the present invention is to provide a composition for preventing, improving and treating liver disorders.


As described above, the development of a medicine having a new action mechanism and effective in preventing, improving and treating metabolic syndrome, particularly liver diseases with abnormal lipid metabolism is demanded.


After intensive investigations made for the purpose of solving the above-described problems, the inventors have found that the elevation of the expression of liver ACL specific for the metabolic syndrome is recognized on the gene expression level in Goto-Kakizaki rats (hereinafter referred to as “GK rats”) which suffer from hyperglycemia caused by insufficient insulin secretion in response to glucose and that surprisingly, when an insulin secretagogue, particularly that having an rapid effect such as a meglitinide, e. g. nateglinide, is administered, elevated liver ACL expression of GK rats can be suppressed. The present invention has been completed on the basis of this finding Diabetes is considered to be one of phenotypes of metabolic syndrome. It was confirmed that when nateglinide was administered for 3 months to patients suffering from diabetes and having fatty liver or mild liver failures, GOT and GPT which are indices of the liver functions of these patients were improved.


Namely, the present invention provides a pharmaceutical composition for suppression of the expression of ACL, which contains a compound suppression of the expression of ACL.


The present invention also provides a composition for preventing, improving and treating metabolic syndrome, which contains a compound suppressing the expression of ACL.


The present invention also provides a composition for preventing, improving and treating fatty liver, which contains a compound suppressing the expression of ACL.


The present invention also provides a composition for preventing, improving and treating NASH, which contains a compound suppressing the expression of ACL.


The present invention also provides a composition for preventing, improving and treating liver disorders, which contains a compound suppressing the expression of ACL.


The present invention also provides use of the above-described compound for producing a composition for preventing, improving and treating metabolic syndrome, fatty liver, NASH and liver disorder.


BEST MODE FOR CARRYING OUT THE INVENTION

The compounds used in the present invention for suppression of the expression of ACL are not particularly limited so far as they have such an effect. In such compounds, those included in meglitinides of the following general formula (I) (Hormone and Metabolic Research Journal, Vol. 27, 263-266 (1995)) are preferred:
embedded image

wherein R1 represents a group represented by the following formula:
embedded image

R2 represents hydrogen atom, a lower alkyl group such as methyl group or ethyl group, R3 represents hydrogen atom, carboxyl group or 1-piperidyl group, A represents NH or CH2 group, and n represents 0 or 1.


More preferred compounds are D-phenylalanine derivatives such as (-)-N-(trans-4-isopropylcyclohexanecarbonyl)-D-phenylalanine (hereinafter referred to as “nateglinide”), benzylsuccinic acid derivatives such as mitiglinide and benzoic acid derivatives such as repaglinide. In them, the most preferred compound is nateglinide:
embedded image


In the present invention, the above-described compounds are usable either alone or in combination with at least one of hypoglycemic agents and therapeutic agent for hyperlipemia. The hypoglycemic agents include, for example, insulin and insulin derivatives such as lispro and glargine, sulfonylureas such as tolbutamide, gliclazide, glibenclamide and glimepiride, a glucosidase inhibitors such as acarbose, voglibose and miglitol, insulin sensitizers such as biguanides, e. g. metformin and phenformin, thiazolidines, e. g. pioglitazone, rosiglitazone and troglitazone and PPAR γ agonists and antagonists having non-thiazolidine structures such as GI-262570, JTT-501, YM-440, NN-622 and KRP-297, adrenaline β3 receptor agonists such as AJ-9677, insulin-like agonists such as CLX-0901, GLP-1 agonists such as GLP-1, Exendin-4 and NN-2211, DPPIV inhibitors such as DPP-728A, SGLT inhibitors such as T-1095 and ACC inhibitors.


The therapeutic agents for hyperlipemia, which lowers blood lipids, include HMG-CoA reductase inhibitors such as pravastatin, simvastatin, fluvastatine, cerivastatin, atorvastatin and itavastatin, fibrate such as simfibrate, clofibrate, clinofibrate, bezafibrate and fenofibrate, anion exchange resins such as colestimide and colestyramine, and nicotinic acid preparations such as nicomol and niceritrol. By using a combination of them, the effect of the present invention can be further improved. Such a combination is very effective on metabolic syndrome, in particular, abnormal lipid metabolism. The term “combination” means either that two of them are contained in a pharmaceutical composition or that two pharmaceutical compositions containing a different ingredient are administered to the patients at the same time or at an interval.


Although the dose of the compound which suppresses the expression of ACL in the pharmaceutical composition, hypoglycemic agent and/or therapeutic agent for hyperlipemia is not particularly limited, the content of the compound which suppresses the expression of ACL in the composition is preferably 0.1 to 99% by weight and that of the hypoglycemic agent and/or therapeutic agent for hyperlipemia is preferably 1 to 99.9% by weight.


The pharmaceutical composition of the present invention can contain, in addition to the above-mentioned ingredients, pharmacologically allowable various substances (as adjuvants) for the preparation (hereinafter referred to as pharmaceutically allowable carriers). The materials for the preparation can be suitably selected depending on the dosage form of the preparation. They include, for example, excipients, diluents, additives, disintegrators, binders, coating agents, lubricants, gliding agent, glazing agents, flavors, sweetening agents and solubilizers. Examples of the materials for the preparation include magnesium carbonate, titanium dioxide, lactose, mannitol and other saccharides, talc, milk protein, gelatin, starch, cellulose and derivatives thereof, animal oils, vegetable oils, polyethylene glycol and solvents such as sterilized water and monohydric or polyhydric alcohols, e. g. glycerol.


The pharmaceutical composition of the present invention is effective for preventing, improving and treating metabolic syndrome. The kinds of the metabolic syndrome for which the pharmaceutical composition is used are not particularly limited, and the composition can be widely used for obesity, fatty liver, NASH, etc. When the pharmaceutical composition of the present invention is used particularly for treating liver diseases, it can be widely used for various liver disorders.


The pharmaceutical preparation of the present invention can be prepared suitably for various administration methods such as oral administration, intraperitoneal administration, percutaneous administration and inhalation administration. Concretely, the pharmaceutical preparation can be in a suitable solid or liquid form such as granules, powder, coated tablets, tablets, (micro)capsules, suppositories, syrup, juice, suspension, emulsion, dropping agent, solution for injection and a preparation capable of elongating the release of the active agent.


The dose of the compound (active ingredient) which suppresses the expression of ACL used for the medicine of the present invention is suitably determined depending on the variety of the compound which suppresses the expression of ACL, kind of complication, extent of the symptoms of the complication and neuropathy, dosage form and side effects of the preparation and degree thereof. For example, when a preparation containing nateglinide as the active ingredient is orally administered, the dose thereof is preferably about 10 mg to 10 g, more preferably about 30 mg to 1 g and most preferably about 90 to 270 mg in terms of the net weight of nateglinide. The dose can be further increased when the patient is under serious conditions. As for the number of times and timing of the medication, the medicine can be administered once/several days or once a day. Usually, the medicine is administered several times a day, for example, 2 to 4 times a day, preferably before meal. In the parenteral administration such as intravenous administration, the dose may be about {fraction (1/10)} to {fraction (1/20)} of the dose in the oral administration.


When one of hypoglycemic agents and therapeutic agents for hyperlipemia is used or when two or more of them are used in the form of a mixture or in combination, the dose or the amount of each of them can be the same as that of the hypoglycemic agent and/or therapeutic agent for hyperlipemia or each of the medicines already developed or being developed as medicines having the intended effects.


The following Examples will further illustrate the present invention.







EXAMPLE1

The effect of nateglinide on the expression of liver ACL was analyzed with DNA chips.


In Experiment 1, methylcellulose or 50 mg/kg of nateglinide suspended in methylcellulose was orally administered to normal Wistar rats fasted overnight. One hour after the administration, the liver was taken from each rat and freezed. The total RNA was extracted with RNeasy kit (Qiagen Co. Ltd). Biotinylated cRNA probe was prepared by a standard method and then it was hybridized to rat genome U34 array (Affymetrix Co. Ltd). The amount of cRNA hybridized to rat ACL gene (GenBank ID: J05210) was analyzed with Microarray Suite 5.0 software (Affymetrix Co. Ltd).


Also in Experiment 2, 1 g/kg of glucose, 50 mg/kg of nateglinide or both of glucose and nateglinide were orally administered to Wistar rats and GK rats fasted overnight. One hour after the administration, the liver was taken from each rat and the expression of ACL level was analyzed with DNA chips in the same manner as that in Experiment 1.

TABLE 1GroupRatGlucose NateglinideAnalysis 1Analysis 2(Experiment 1)1Wistar96.2459.32Wistar+144.4543.6(Experiment 2)1Wistar79.2257.32Wistar+63.52823GK139.6452.54GK rat+139.6416.75GK rat++66.4189.9


The expression level of liver ACL was constitutively elevated in GK rats as compared with normal Wistar rats (Experiment 2, lvs3).


It is considered that the load of glucose on normal rats increases the blood glucose level and also causes normal portal insulin secretion. However, even when normal rats were exposed to high glucose and high insulin, the expression level of liver ACL genes was not suppressed one hour after the administration (Experiment 2, lvs2). Also in GK rats, no significant change was found in the expression of liver ACL by the load with glucose (Experiment 2, 3vs4). When nateglinide was administered to normal Wistar rats, no significant suppression of liver ACL mRNA level was recognized (Experiment 1).


On the contrary, when nateglinide was administered to GK rats (Experiment 2, 3,4vs5), surprisingly, the elevated ACL expression level was significantly suppressed and returned to the normal level. By the administration of nateglinide, transient increase in insulin level in GK rat portal vein was observed.


Thus, it was confirmed that by the administration of nateglinide, the elevated liver ACL expression level of GK rats was remarkably improved.


EXAMPLE 2

Nateglinide was orally administered to patients with type 2 diabetes three times a day in a dose of usually 90 mg/day before meals for 12 weeks. Blood GOT and GPT concentrations were determined as indices of the liver function in 0 week and 12th week.


In analysis 1, the results obtained by the oral administration of nateglinide to 53 patients with type 2 diabetes each having fatty liver for 12 weeks were analyzed. The results are shown in Table 2.

TABLE 20 week12th weekcustom character(0 to 12 weeks)pGOT (IU/L)58.4 ± 34.433.8 ± 22.924.7 ± 12.4<0.05GPT (IU/L)77.2 ± 55.944.0 ± 29.733.2 ± 31.0<0.05


Levels of GOT and GPT after the administration of nateglinide statistically significant lowered, compared with those before the administration thereof.


In 5 cases with fatty liver and having NASH-like liver troubles (GOT, GPT≧51 IU/L, GPT>GOT,), GOT value was reduced from 138.6±56.0 to 83.6±41.5, and GPT value was reduced from 242.6±112.8 to 57.8±59.2.


In analysis 2, the results obtained by the oral administration of nateglinide to 16 cases of type-2 diabetes having liver disorders (GOT, GPT≧51 IU/L) were analyzed. The results are shown in Table 3.

TABLE 30 week12th weekcustom character(0 to 12 weeks)pGOT (IU/L)133.3 ± 51.385.4 ± 40.9 47.8 ± 37.9<0.05GPT (IU/L)217.3 ± 94.180.2 ± 53.4137.0 ± 43.4<0.05


In the comparison of GOT and GPT before the administration of nateglinide with those after the administration thereof, a statistically significant lowering in both GOT and GPT was recognized.


It was thus suggested that the liver function of patients with fatty liver, NASH or liver disorders can be improved by the administration of nateglinide.


Thus, nateglinide can be expected as a medicine for the prevention, improvement or treatment of liver disorders caused by metabolic syndrome, particularly abnormal lipid metabolism.


The present invention can provide medicines for the prevention, improvement, treatment, etc. of metabolic syndrome, fatty liver, NASH and liver disorders, methods for using the medicines (e. g. method of the administration for the treatment of these diseases) and use of the compounds, capable of suppression of ACL expression for this purpose, for the preparation of the medicine. In particular, nateglinide is expected as the compound for suppression of the expression of ACL.

Claims
  • 1. A pharmaceutical composition for suppression of the expression of ATP citrate lyase, which contains a compound controlling the expression of ATP citrate lyase.
  • 2. The pharmaceutical composition according to claim 1, wherein the compound for controlling the expression of ATP citrate lyase is an insulin secretagogue.
  • 3. The pharmaceutical composition according to claim 1, wherein the compound for controlling the expression of ATP citrate lyase is a rapid-acting insulin secretagogue.
  • 4. The pharmaceutical composition according to claim 3, wherein the rapid-acting insulin secretagogue is a meglitinides.
  • 5. The pharmaceutical composition according to claim 3, wherein the rapid-acting insulin secretagogue is nateglinide.
  • 6. The pharmaceutical composition according to claim 1, which suppresses the expression of liver ATP citrate lyase elevated by diabetes by the in vivo administration.
  • 7. A pharmaceutical composition for preventing, improving or treating metabolic syndrome, which contains a compound of claim 1 as the active ingredient.
  • 8. A pharmaceutical composition for preventing, improving or treating fatty liver, which contains a compound of claim 1 as the active ingredient.
  • 9. A pharmaceutical composition for preventing, improving or treating NASH, which contains a compound of claim 1 as the active ingredient.
  • 10. A pharmaceutical composition for preventing, improving or treating liver disorder, which contains a compound of claim 1 as the active ingredient.
  • 11. The pharmaceutical composition of claim 1 which further contains at least one of hypoglycemic agents or therapeutic agents for hyperlipemia.
  • 12. The pharmaceutical composition for suppression of the expression of ATP citrate lyase which comprises a combination of a compound of claim 1 and at least one of hypoglycemic agents or therapeutic agents for hyperlipemia.
  • 13. A method of preventing, improving and/or treating metabolic syndrome, which comprises administering a compound of claim 1 to a patient.
  • 14. A method of claim 13 wherein said compound is administered thereto in combination with at least one of hypoglycemic agents or therapeutic agents for hyperlipemia.
  • 15. A method of preventing, improving and/or treating fatty liver, which comprises administering a compound of claim 1 to a patient.
  • 16. A method of claim 15 wherein said compound is administered thereto in combination with at least one of hypoglycemic agents or therapeutic agents for hyperlipemia.
  • 17. A method of preventing, improving and/or treating NASH, which comprises administering a compound of claim 1 to a patient.
  • 18. A method of claim 17 wherein said compound is administered thereto in combination with at least one of hypoglycemic agents or therapeutic agents for hyperlipemia.
  • 19. A method of preventing, improving or treating liver disorders, which comprises administering a compound of claim 1 to a patient.
  • 20. A method of claim 19 wherein said compound is administered thereto in combination with at least one of hypoglycemic agents or therapeutic agents for hyperlipemia.
Priority Claims (1)
Number Date Country Kind
2002-154397 May 2002 JP national
Continuations (1)
Number Date Country
Parent PCT/JP03/06651 May 2003 US
Child 10997873 Nov 2004 US