AU2001245785A1

AU2001245785A1 - Method for treating congestive heart failure

Info

Publication number: AU2001245785A1
Application number: AU2001245785A
Authority: AU
Inventors: Irwin Klein; Kaie Ojamaa
Original assignee: North Shore Long Island Jewish Research Institute
Current assignee: Feinstein Institutes for Medical Research
Priority date: 2000-03-23
Filing date: 2001-03-16
Publication date: 2001-12-13
Anticipated expiration: 2021-03-16

Description

METHOD FOR TREATING CONGESTIVE HEART FAILURE

Background of the Invention

Congestive heart failure (CHF) is a common syndrome characterized by decreased cardiac contractility, abnormal diastolic compliance, reduced stroke volume, and pulmonary congestion, as well as decreased cardiac output. CHF may be caused by many different etiologies whose clinical manifestations reflect a decrease in the myocardial contractile state such that cardiac output is reduced. The CHF disease state may arise, for example, from deficiencies in cardiac contractility, right ventricular failure, biventricular failure, systolic dysfunction, diastolic dysfunction, and pulmonary effects. In particular, CHF develops when plasma volume increases and fluid accumulates in the lungs, abdominal organs, and peripheral tissues (Beers and Berkow, eds., The Merck Manual of Diagnosis and Therapy, 17^th ed. (Whitehouse Station, NJ: Merck Research Laboratories, 1999) 1682-88).

Drug treatment for CHF primarily involves diuretics, ACE inhibitors, digitalis, and β-blockers. In mild cases, thiazide diuretics, such as hydrochlorothiazide at 25-50 mg/day or chlorothiazide at 250-500 mg/day, are useful. However, supplemental potassium chloride is generally needed, since chronic diuresis causes hypokalemis alkalosis. Moreover, thiazide diuretics usually are not effective in patients with advanced symptoms of CHF. Typical doses of ACE inhibitors include captopril at 25-50 mg/day and quinapril at 10 mg/day. Numerous side effects are possible, though, including decreased blood pressure, renal insufficiency, potassium retention, and coughing. Digitalis preparations, particularly of digoxin, are widely prescribed in the United States, although the role of digitalis continues to be debated, and its usefulness in treating CHF in the absence of atrial fibrillation remains controversial, β- blockers, too, must be used with caution when treating patients with CHF. A more indirect component of CHF management includes the recognition and control of factors that may be causing increased cardiac demands or adversely affecting myocardial function (e.g., hypertension, anemia, excess salt intake, excess alcohol, arrhythmias, thyrotoxicosis, fever, increased ambient temperature, or pulmonary emboli) (Beers and Berkow, eds., The Merck Manual of Diagnosis and Therapy, 17^th ed. (Whitehouse Station, NJ: Merck Research Laboratories, 1999) 1688-91). In view of the foregoing, many of the current methods available for treating CHF produce negative side-effects, or are only indirect. Accordingly, there currently exists a need for new and better methods for improving the survival of patients with CHF. Triiodothyronine (T₃) is a hormone synthesized in the thyroid gland.

Along with tetraiodothyronine (T₄), T₃ is produced by the iodination and coupling of the amino acid tyrosine. T₃ is known to enhance oxygen (O₂) consumption by most tissues of the body, increase the basal metabolic rate, and influence the metabolism of carbohydrates, lipids, and proteins. While T₄ is commonly administered in replacement or supplemental therapy to treat patients with most forms of hypothyroidism, T₃ is only rarely administered because numerous complications are associated with its usage (as discussed below) . In addition, T₃ is used as a pituitary thyroid-stimulating hormone (TSH) suppressant, in the treatment or prevention of various types of euthyroid goiters. Finally, T₃ is used as a diagnostic agent in suppression tests to differentiate suspected mild hyperthyroidism or thyroid gland autonomy (Physicians' Desk Reference, 54^th ed. (Montvale, NJ: Medical Economics Company, Inc., 2000) 1081, 1513).

Studies have also demonstrated that acute administration of T₃ can result in increased cardiac performance and reduced systemic resistance in a number of clinical scenarios, including cardiac transplantation, cardiopulmonary bypass (Klemperer et al, N. Engl J. Med., 333:1522-27, 1995), and myocardial ischemia (a deficiency of blood supply to the heart muscle, due to obstruction or constriction of coronary arteries) (Klein et al., Hosp. Formal., 28:848-58, 1993). Nevertheless, it is well-recognized that thyroid-hormone therapy should be used with great caution in a number of circumstances where the integrity of the cardiovascular system, particularly the coronary arteries, is suspected (Physicians' Desk Reference, 54^th ed. (Montvale, NJ: Medical Economics Company, Inc., 2000) 1082, 1513). Indeed, the long-term or chronic administration of T₃ has been historically contraindicated, due to concerns regarding oxygen-wasting effects, arrhythmia, and exacerbation of angina pectoris. In particular, the prevalent paradigm holds that T₃ is not suitable for long-term treatment, as it increases O₂ consumption by the heart without a concomitant increase in the blood supply: a classic scenario for the development of angina, fibrillation, and other heart conditions (Levine, H.O., Am. J. Med., 69:411-18, 1980; Klemperer et al, N. Engl J. Med., 333:1522-27, 1995; and Klein and Ojamaa, Am. J. Cardiol, 81: 490-91, 1998). H.D. Levine (Am. J. Med., 69:411-18, 1980), for example, even suggested that the administration of thyroid hormone, and the return to a euthyroid state, would actually induce or exacerbate heart problems in patients with hypothyroidism and coronary disease.

The possible use of thyroid hormone to treat CHF was considered by Klein and Ojamaa in a review article (Am. J. Cardiol, 81: 490-91, 1998). The suggestion was based predominantly on an earlier study in which a single high dose of thyroid hormone was administered to improve cardiac performance in an acute setting. No evidence was provided to indicate that long-term administration of T₃ could be successfully and safely used to treat CHF. The authors also expressly acknowledged that further research was necessary to ascertain the safety and efficacy of the use of T₃ to treat CHF. In view of the known contraindications associated with the long-term administration of T₃, the skilled artisan would not have had a reasonable expectation that T₃ could be used to safely treat CHF. Summary of the Invention

The present invention is predicated on the discovery that, contrary to the expectations in the prior art which teach away from the long-term T₃ administration, T₃ can successfully be used to treat CHF without producing deleterious effects. On the basis of this finding, the present invention provides a method for chronic treatment of congestive heart failure (CHF) by administering to the patient, over the long term, a daily dose of T₃.

Additional objects of the present invention will be apparent in view of the description which follows.

Brief Description of the Figure Figure 1 depicts a time line for the experimental protocol utilized on animals in the present invention. As the figure illustrates, the animal's coronary artery was ligated by surgery, inducing myocardial infarction (MI). Two weeks later, T₃ administration was commenced. Two weeks after the commencement of T₃ administration, the percent ejection fraction (% EF) of the animal was measured in order to assess the function of the heart. One week later, % EF was again measured in the MI animal.

Detailed Description of the Invention

The present invention is directed to a method for chronic treatment of congestive heart failure (CHF) in a patient having CHF. The method of the present invention comprises the long-term administration to a patient of a daily dose of T₃ effective to treat CHF. The term "treat CHF", as used herein, means treating any one or more of the conditions underlying CHF, including, without limitation, decreased cardiac contractility, abnormal diastolic compliance, reduced stroke volume, pulmonary congestion, and decreased cardiac output, while minimizing or attenuating deleterious effects commonly associated with the long-term administration of T₃, such as oxygen-wasting effects, arrhythmias, and exacerbation of angina pectoris. As further used herein, "oxygen-wasting effects" include, without limitation, symptoms and signs of congestion due to increased ventricular filling pressures, and fatigue associated with low cardiac output.

As used herein, "long-term administration" means administration for at least three weeks. Furthermore, as used herein, "a daily dose" means the dose given within a 24-hour period. Additionally, as used herein, "T₃" refers to triiodothyronine and analogues thereof, including, for example, a functional variant of T₃ which has T₃ biological activity, as well as a fragment of T₃ having T₃ biological activity. As further used herein, the term "T₃ biological activity" refers to T₃ activity which improves myocardial contractility in a patient having CHF.

Synthetic T₃ is commercially available, and can be obtained from Jones Pharma Incorporated (St. Louis, MO). Liothyronine sodium is a synthetic preparation of T₃, and can be purchased in oral (Cytomel) and intravenous (Triostat) formulations. Cytomel tablets contain liothyronine (L- triiodothyronine), a synthetic form of a natural thyroid hormone, that is available as the sodium salt (Physicians' Desk Reference, 54^th ed. (Montvale, NJ: Medical Economics Company, Inc., 2000) 1467). A natural preparation of T₃ may be derived from animal thyroid. Natural preparations include desiccated thyroid and thyroglobulin. Desiccated thyroid is derived from domesticated animals that are used for food by humans (e.g., beef or hog thyroid), and thyroglobulin is derived from thyroid glands of the hog.

According to the method of the present invention, the amount of T₃ administered to a patient is a dose effective to treat CHF in a patient. It is an objective of the present invention to administer a dose of T₃ which will treat the conditions underlying CHF, including, without limitation, decreased cardiac contractility, abnormal diastolic compliance, reduced stroke volume, pulmonary congestion, and decreased cardiac output, while minimizing, attenuating or reducing deleterious effects commonly associated with the long-term administration of T₃, such as oxygen-wasting effects, arrhythmias, and exacerbation of angina pectoris. Preferably, the dose of T₃ is such that deleterious effects commonly associated with the long-term administration of T₃ are eliminated.

The method of the present invention may be used to treat a patient who is T₃-deficient, as well as a patient who is not T₃-deficient. However, it is preferable that T₃ be administered to a patient who is deficient in T₃. In such a patient, low doses of T₃, administered over the long term, would be expected to normalize, or slightly elevate above normal, serum T₃ levels in the patient, with minimal or no deleterious effects commonly associated with the long-term administration of T₃.

In the method of the present invention, T₃ is preferably administered chronically at a dose between about 5 μg/day and about 50 μg/day (i.e., between about 0.07 μg/kg/day and about 0.71 μg/kg/day). However, the actual dose will depend on the particular factors of each case, including the patient's weight and the severity of the patient's condition. Most preferably, T₃ is administered at a dose between about 15 μg/day and about 30 μg/day (i.e., between about 0.21 μg/kg/day and about 0.43 μg/kg/day). This amount of T₃ is extremely low compared to that required for acute treatment of heart failure patients and post-operation cardiac patients, for example, where T₃ is administered intravenously at a dose between 100 μg and 150 μg, over a 12- hour period.

According to the method of the present invention, the dose of T₃ is preferably administered daily for at least three weeks. The administration of T₃ may continue as long as the patient has symptoms of CHF and derives benefit from the administration of T₃. It is within the confines of the present invention that the T₃ be administered to the patient throughout his or her lifetime. The dose of T₃ may be administered to a human or animal patient by known procedures, including, but not limited to, oral administration, injection, transdermal administration, and administration through an osmotic mini-pump. Preferably, the dose of T₃ is administered orally. For oral administration, the formulation of the dose of T₃ may be presented as capsules, tablets, powders, granules, or as a suspension. Preferably, the dose of T₃ is presented in a known sustained-release formulation, such that a single daily dose of T₃ may be administered. Specific sustained- release formulations are described in U.S. Patent Nos. 5,885,616, 5,922,356, 5,968,554, 6,011,011, and 6,039,980, which are hereby incorporated by reference. The formulation of T₃ may have conventional additives, such as lactose, mannitol, corn starch, or potato starch. The formulation may also be presented with binders, such as crystalline cellulose, cellulose derivatives, acacia, corn starch, or gelatins. Additionally, the formulation may be presented with disintegrators, such as corn starch, potato starch, or sodium carboxymethyl-cellulose. Finally, the formulation may be presented with lubricants, such as talc or magnesium stearate.

For injection, the dose of T₃ may be combined with a sterile aqueous solution which is preferably isotonic with the blood of the patient. Such a formulation may be prepared by dissolving a solid active ingredient in water containing physiologically-compatible substances, such as sodium chloride, glycine, and the like, and having a buffered pH compatible with physiological conditions, so as to produce an aqueous solution, then rendering said solution sterile. The formulations may be present in unit or multi-dose containers, such as sealed ampoules or vials. The formulation may be delivered by any mode of injection, including, without limitation, epifascial, intracutaneous, intramuscular, intravascular, intravenous, parenchymatous, or subcutaneous. For transdermal administration, the dose of T₃ may be combined with skin penetration enhancers, such as propylene glycol, polyethylene glycol, isopropanol, ethanol, oleic acid, N-methylpyrrolidone, and the like, which increase the permeability of the skin to the dose of T₃, and permit the dose of T₃ to penetrate through the skin and into the bloodstream. The T₃/enhancer compositions may also be further combined with a polymeric substance, such as ethylcellulose, hydroxypropyl cellulose, ethylene/vinylacetate, polyvinyl pyrrolidone, and the like, to provide the composition in gel form, which may be dissolved in solvent such as methylene chloride, evaporated to the desired viscosity, and then applied to backing material to provide a patch.

The dose of T₃ of the present invention may also be released or delivered from an osmotic mini-pump. The release rate from an elementary osmotic mini- pump may be modulated with a microporous, fast-response gel disposed in the release orifice. An osmotic mini-pump would be useful for controlling release, or targeting delivery, of T₃.

The present invention is described in the following Experimental Details section, which is set forth to aid in the understanding of the invention, and should not be construed to limit in any way the scope of the invention as defined in the claims which follow thereafter.

Experimental Details An animal model of myocardial infarction was used in the present studies to produce a model of CHF in which a decrease in serum T₃ could be demonstrated. This model was used to test the hypothesis that long-term, low- dose T₃ treatment could improve cardiac function. Analysis of the cardiac tissue was conducted to determine the molecular mechanisms by which this effect occurs.

Animals subjected to ligation of a coronary artery developed myocardial infarction (MI) and a decrease in function of the heart, as measured by the percent ejection fraction (% EF) (stroke volume/end-diastolic volume - normally >50%). As Table 1 shows, serum total T₃ levels in the MI animals fell by 40%, as compared with 56.58 ± 8.35 ng/dl in the controls (C). This result was analogous to the decrease in serum total T₃ levels observed in humans. In the MI animals, % EF decreased by 47% over 14 and 21 days after surgery (Table 2). Table 1. Serum total T₃ and total T₄ in control (C) rats, myocardial infarcted (MI) rats, and MI rats treated with T₃ (MI + T₃)

* p<0.05 vs. C and MI + T₃ ** p<0.05 vs. C and MI T₃ was administered by continuous subcutaneous infusion to a subset of the MI animals, 2 weeks after coronary artery ligation surgery (Figure 1). At the low-dose T₃ treatment regimen, measurements of serum total T₃ levels were restored to normal values at the termination of the experiment (Table 1). At the same time, serum T₄ levels fell, reflecting the expected effect of T₃ on the pituitary-thyroid axis (Table 1). As Table 2 shows, T₃ treatment produced a time-dependent increase in % EF in the MI animals (MI + T₃), and returned left ventricular function to 80% of control (C) animals (65 ± 2 vs. 82 ± 2 % EF), as compared with 59% of controls in the untreated MI animals.

Table 2. Effects of T₃ treatment on ejection fractions (% EF) of rats with myocardial infarction (MI)

% EF measured by M-mode echo

* p<0.01 vs. C ** p<0.05 vs. MI Cardiac contractility is primarily regulated by the calcium cycling proteins: sarcoplasmic reticulum (SR) calcium-ATPase (SERCA2) and phospholamban (PLB). T₃ is known to regulate these proteins in normal hearts. As Table 3 shows, chronic subcutaneous administration of T₃ increased SERCA2 protein content in MI hearts, and altered the ratio of SERCA2 to PLB in a direction that can account for the increase in % EF. In addition, T₃ treatment of MI animals altered the PLB phosphorylation state (1.6 vs. 1.0 PLB- phos/unphos), which is also an established mechanism to enhance contractility of the heart.

Based on the above data, it may be concluded that chronic T₃ treatment can be proposed as a therapy for improvement of cardiac function in a variety of disease states, including CHF.

Table 3. Western analysis of SR calcium-ATPase and phospholamban in response to myocardial infarction (MI) and T₃ treatment (MI +

T₃)

* p<0.05 vs. G and MI ** p<0.05 vs. C

All publications mentioned hereinabove are hereby incorporated in their entirety. While the foregoing invention has been described in some detail for purposes of clarity and understanding, it will be appreciated by one skilled in -lithe art, from a reading of the disclosure, that various changes in form and detail can be made without departing from the true scope of the invention in the appended claims.

Claims

What is claimed is:

1. A method for treating congestive heart failure (CHF) in a patient having CHF, comprising the long-term administration to the patient an amount of T₃ effective to treat CHF in the patient.

2. The method of Claim 1, wherein T₃ is administered daily.

3. The method of Claim 1, wherein T₃ is administered at a dose between about 5 μg/day and about 50 μg/day.

4. The method of Claim 1, wherein T₃ is administered at a dose between about 15 μg/day and about 30 μg/day.

5. The method of Claim 1, wherein T₃ is administered for at least three weeks.

6. The method of Claim 1, wherein T₃ is administered orally.

7. The method of Claim 1, wherein T₃ is administered once daily in a sustained-release formulation.

8. An oral pharmaceutical composition comprising 5 μg to 15 μg of T₃ and a sustained-release formulation.