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==Overview==
==Overview==
There is a direct relationship between levels of circulating LDL cholesterol and the risk of cardiovascular disease.  There is an unmet need for more effective and tolerable therapies for reducing LDL-C, which is a direct consequence of failures observed with the available therapies at achieving target LDL-C levels.  This section describes novel therapeutic targets currently under development, including anti-sense oligonucleotides (ASOs) to apolipoprotein B (apo B), proprotein convertase subtilisin/kexin type 9 ([[PCSK9]]), microsomal triglyceride transfer protein (MTP), thyromimetics, [[squalene synthase]], adenosine triphosphate-citrate lyase, [[AMP-activated protein kinase]], and [[sterol regulatory element binding protein]]s.
There is a direct relationship between levels of circulating LDL cholesterol and the risk of cardiovascular disease.  There is an unmet need for more effective and tolerable therapies for reducing LDL-C, which is a direct consequence of failures observed with the available therapies at achieving target LDL-C levels.  This section describes novel therapeutic targets currently under development, including anti-sense oligonucleotides (ASOs) to apolipoprotein B (apo B), proprotein convertase subtilisin/kexin type 9 ([[PCSK9]]), [[microsomal triglyceride transfer protein]] (MTP), thyromimetics, [[squalene synthase]], adenosine triphosphate-citrate lyase, [[AMP-activated protein kinase]], and [[sterol regulatory element binding protein]]s.


==The Unmet Need Driving Research into Lowering LDL==
==The Unmet Need Driving Research into Lowering LDL==

Revision as of 21:47, 25 November 2013

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Ayokunle Olubaniyi, M.B,B.S [2]

Overview

There is a direct relationship between levels of circulating LDL cholesterol and the risk of cardiovascular disease. There is an unmet need for more effective and tolerable therapies for reducing LDL-C, which is a direct consequence of failures observed with the available therapies at achieving target LDL-C levels. This section describes novel therapeutic targets currently under development, including anti-sense oligonucleotides (ASOs) to apolipoprotein B (apo B), proprotein convertase subtilisin/kexin type 9 (PCSK9), microsomal triglyceride transfer protein (MTP), thyromimetics, squalene synthase, adenosine triphosphate-citrate lyase, AMP-activated protein kinase, and sterol regulatory element binding proteins.

The Unmet Need Driving Research into Lowering LDL

Although the relative rate of death attributable to cardiovascular disease declined by 32.7% in the past decade, the burden of disease remains very high at 1 out of every 3 deaths in the United States,[1] and the direct medical cost is expected to triple by 2030.[2] LDL cholesterol remains the dominant determinant of cardiovascular heart diseases,[3] thus making statins (HMG CoA reductase inhibitors) central in the fight against atherosclerosis. However, 40% and 80% of individuals with high- and very-high cardiovascular risk, respectively, still do not achieve their LDL-C goals with optimal doses of statins.[4] Therefore, alternative therapeutic targets to effectively and safely reduce LDL cholesterol are actively being investigated.

Investigational Therapies

Inhibition of Apolipoprotein B Production

Apolipoprotein B (apo B) is a large protein that is present in all atherogenic lipoproteins i.e., VLDL, LDL, IDL. There is a single copy of apo B-100 in all these lipoproteins, therefore plasma levels of apo B-100 is proportionate to the concentration of circulating atherogenic lipoproteins and a predictor of cardiovascular risk.[5] From the apoB gene, the liver synthesizes apo B-100; and the intestine synthesizes apo B-48 which is required for chylomicron assemly and fat absorption. The apo B-100 serves two functions - provides structural stability to the circulating lipoproteins as well as acts as a ligand for LDL receptors (LDLR). The removal of LDL from the plasma involves the binding of apo B to LDLR, then, the resulting apo B-100-LDLR complex gets internalized into the liver for processing.[6] Mutations that lower the affinity of apo B-100 for LDLR result in decreased clearance of LDLs, a condition known as familial defective apo B with an increased risk of atherosclerotic cardiovascular diseases.[7][8] In contrast, mutations in apo B that decrease its translation or secretion, or increase its breakdown have been demonstrated to reduce the circulating LDL-C and improve cardiovascular risk.[9]

The DNA contains two strands - 'sense' and 'antisense' which run complementary to each other. The antisense strand encodes a sequence of events that initiates protein synthesis and production of messenger RNA (mRNA) which later serves as a template for protein synthesis through a process called translation. Antisense oligoneucleotides (ASOs) are short, deoxyribonucleotide strands which bind to the targeted mRNAs to inhibit gene expression. They can inhibit mRNA translation and mRNA splicing leading to its enzymatic degradation by ribonuclease (RNAse H or argonaute 2); inhibit translation or prevent the maturation of mRNA.[10]

ISIS 301012 or mipomersen, by ISIS Pharmaceuticals, is a second-generation 20 nucleotide ASO which selectively inhibits apo B gene expression via RNAse H activation.[11] Phases I and II clinical trials have demonstrated a dose-dependent reduction of plasma apo B levels by 40% and up to 50% reduction in LDL-C of a subcutaneously administered ISIS-301012 or mipomersen, even with a defective LDLR.[12][13][14] Furthermore, a phase III randomized clinical trial involving homozygous FH revealed a 15% elevation in HDL-C.[15] Despite its efficacy in lowering LDL-C, its approval have been hampered with the development of adverse effects - injection site reactions (80-100% of patients), flu-like illness, and 3-fold elevation in liver transaminases (15%).

PCSK9 Inhibition

PCSK9 has a major role in the metabolism of hepatic cholesterol. It is a serine protease which binds to the epidermal growth factor-like repeat A (EGF-A) domain of the low-density lipoprotein receptor (LDLR), inducing LDLR degradation in the lysosomes. Reduced LDL receptor levels result in decreased metabolism of low density lipoprotein (LDL), which could lead to hypercholesterolemia.[16] The sterol regulatory element-binding protein-2 (SREBP-2), which is activated in the presence of low intracellular levels of cholesterol, also induces the expression of PCSK9, thereby increasing the amount of circulating LDL-cholesterol.[17] In addition to the effect on LDL-C, PCSK9 deficiency has also been shown to lower cardiovascular risk factors by reducing postprandial triglyceridemia.[18] In another study, PCSK9-deficient mice were also demonstrated to have a reduced lymphatic apoB secretion,[19] as well as an increased ability to clear chylomicrons.

For more information regarding this novel approach to lipid management, Click here.

Microsomal Triglyceride Transfer Protein (MTP) Inhibition

Microsomal triglyceride transfer protein is an endosomal protein found in the hepatocytes and intestinal enterocytes. It catalyses the transfer of cholesterol esters and triglycerides to nascent apo B, leading to the formation of chylomicron and VLDL in the intestine and hepatocyte respectively.[20] Chylomicrons and other apo-B48-containing remnant lipoproteins are essential for intestinal fat absorption and its transfer to peripheral tissues. Mutations of the MTTP gene leads to a condition known as abetalipoproteinemia, which causes an absence of apo-B-containing lipoproteins and very low levels of LDL-C and triglycerides.[21][22] Individuals with this recessive condition have severe intestinal malabsorption of fat and fat-soluble vitamins (A, D, E, K) manifesting as fatty liver, night-blindness, rickets or osteomalacia, neuropathy, ataxia, and coagulopathy.

Many MTP inhibitors are being investigated, including non-intestinal specific agents such as lomitapide (AEGR-427, previously known as BMS-201038 - Bristol-Myers-Squibb) by Aegerion Pharmaceuticals, implitapide (formerly AEGR-427 or Bayer BAY-13-9952), and CP-34086 by Pfizer; intestinal specific agents such as dirlotapide (by Pfizer), JTT-130, and SLx-4090 by Surface Logix. A clinical trial assessing the efficacy of lometapide in 6 patients with homozygous familial hypercholesterolemia demonstrated a 58%, 51%, and 55% reductions in total cholesterol, LDL-C and apo B respectively.[23] Higher doses were associated with a transient elevation of liver transaminases and hepatic fat. A double-blinded, randomized controlled trial involving 84 subjects further demonstrated a 20%, 30%, and 46% reduction in LDL-C in ezetimide alone, lometapide alone, and lometapide plus ezetimide combination study groups respectively, further emphasizing the beneficial effect of lometapide monotherapy or in combination therapy was associated with significantly greater reductions in LDL-C levels compared with ezetimibe monotherapy.[24] Another MTP inhibitor, CP-34086 by Pfizer, showed a 47% and 72% reduction in total cholesterol and LDL-C in healthy human volunteers respectively.[25] Currently, further developments of CP-34086 and implitapide have been placed on hold due to their hepatic adverse effects.

Intestinal-specific agents such as dirlotapide, JTT-130, and SLx-4090 were developed to prevent the hepatic effects of the non-specific agents. Thus far, they are still early in human clinical trials (except dirlotapide) but there were reports of significant reductions in postprandial triglyceridemia and total cholesterol in preclinical animal studies with dirlotapide.[26] Intestinal-specific MTP inhibitors may be effective in treating hyperchylomicronemia but their efficacy as LDL-C lowering agents is uncertain.

Thyromimetics

The association between thyroid hormones and cholesterol metabolism was first discovered by Mason in the 1930s, and its use as a cholesterol lowering agent has been investigated in several studies.[27][28][29] However, their development had been hindered by the associated adverse cardiac effects, which was mainly due to the contamination of the investigated thyroid hormone, dextrothyroxine (DT4) with levothyroxine (LT4),[30][31] and by the birth of statins. The recent discovery of thyroid hormone receptors (TRs) have brought this approach back into existence. There are two main TRs in humans:

  • TRα receptors (TRα 1 & 2). TRα 1 is predominantly in the muscles and adipose tissue; also mediates the cardiovascular responses to thyroid hormones such as tachycardia.[32]
  • TRβ receptors (TRβ 1 & 2). TRβ 1 is mainly in the liver and it regulates cholesterol homeostasis.[32] Therefore, the development of TRβ 1-specific thyromimetic would be a promising method of cholesterol management devoid of cardiac effects.[33][34]

Some of the proposed mechanisms of action of these agents include:

  • Upregualtion of hepatic LDLR expression by TRβ.[35][36]
  • Stimulation of bile acid synthesis through the upregulation of the rate-limiting enzyme, cholesterol 7-hydroxylase [CYP7A1])
  • Stimulation of biliary excretion (through increased expression of ATP-binding cassette proteins G5/G8 [ABCG5/G8]
  • Promotion of reverse cholesterol transport which ultimately increases the formation of HDL, enhances cholesteryl ester transfer protein (CETP) activity, and increases scavenger receptor B-I (SR-BI) activity for the uptake of cholesterol.

Examples of TRβ 1-specific thyromimetics that had been investigated include:

  • DITPA (3,5-diiodothyropropionic acid) - terminated
  • Eprotirome (KB2115)[37] by Karo Bio AB.
  • Sobetirome (GC-1)
  • MB07811
  • KB-141
  • T-0681

Squalene Synthase Inhibition

Similar to the statins (3-hydroxy-3-methylglutaryl-CoA reductase inhibitors), inhibitors of squalene synthase prevent the conversion of farnesyl pyrophosphate to squalene at a point on the HMG-CoA-Mevalonate pathway which represents the commitment of cholesterol intermediates to the synthesis of cholesterol. Squalene synthase inhibitors have been shown to inhibit cholesterol production, reduce triglyceride synthesis and apoB secretion, increase LDL receptor expression and LDL uptake in HepG2 cells.[38] However, they are less likely to be associated with the adverse myopathic effects commonly observed with statins because they do not cause depletion of isoprenoid intermediates within the cholesterol biosynthesis pathway, and as a result, they do not limit the prenylation or lipidation (addition of hydrophobic molecules to a protein) of membrane-directed proteins.[39]

TAK-475 (lapaquistat acetate) by Takeda Pharmaceuticals was the first squalene synthase inhibitor to reach phase III clinical trials for the treatment of hypercholesterolemia in the United States and Europe. Randomized, double-blinded, placebo and actively controlled, parallel-group studies involving TAK-475 alone and in combination with atovastatin were associated with a dose-dependent reduction of LDL-C up to 27% and 19% when compared with placebo and when combined with atovastatin, respectively in healthy human volunteers. Recent animal studies have demonstrated a protective effect against statin-induced myopathy when isoprenoid intermediates are replenished directly or by the use of TAK-475 given with high-dose statins.[40] Results from these studies further underscore squalene synthase inhibitors as potential drugs to clinically prevent statin-induced myopathies.

Phase III multi-centered clinical trials are on-going to compare TAK-475 vs simvastatin alone or in combination, vs. ezetimibe, and as add-on in patients already on atorvastatin, rosuvastatin, or a low or high-dose statin. It will also be investigated as add-on treatment in patients with homozygous familial hypercholesterolemia, and in patients with type 2 diabetes.

Inhibition of ACL and Activation of AMPK

ETC-1002 (8-hydroxy-2,2,14,14-tetramethylpentadecanedioic acid), by Esperion Therapeutics, is a small molecule which regulates lipid and carbohydrate metabolism. It modulates the activity of two distinct molecular targets - hepatic adenosine triphosphate-citrate lyase (ACL) and AMP-activated protein kinase (AMPK).[41] It works by:

  • Inhibition of ACL - Inhibition of adenosine triphosphate-citrate lyase, an enzyme responsible for the production of ATP citrate, reduces the levels of acetyl co-enzyme A (acetyl-CoA - an important precursor to HMG-CoA which is a vital component in cholesterol and ketone synthesis). It acts on the lipid synthesis pathway upstream of HMG CoA reductase - the molecular targets of statins.[42]
  • Activation of adenosine monophosphate activated protein kinase (AMP-activated protein kinase) - AMP-activated protein kinase is a functional enzyme present in the liver, striated muscle, and the brain. It plays a key role in cellular energy homeostasis. It acts as a sensor of the energy-depleted form of ATP (i.e., AMP), and its activation results in stimulation of hepatic fatty acid oxidation and ketogenesis, inhibition of cholesterol synthesis, lipogenesis, and triglyceride synthesis, inhibition of adipocyte lipolysis and lipogenesis, stimulation of skeletal muscle fatty acid oxidation and muscle glucose uptake,[43] and modulation of insulin secretion by pancreatic beta-cells.[44]

In a phase II clinical trial involving 177 patients, ETC-1002 was shown to have a dose-dependent reduction of up to 27% in LDL-C (compared with placebo) observed with the maximum dose (120mg), devoid of serious adverse effects.[42] This approach may represent a new target mechanism to reducing LDL-C, but additional studies are required to determine the safety due to its high possibility of producing similar adverse effects as statins.

Inhibition of SREBP-1

Sterol regulatory element binding proteins (SREBPs) are transcription factors required in the activation of genes involved in cholesterol and fatty acid biosynthesis. Fatostatin, a diarylthiazole derivative, was observed to impair the activation of SREBPs, thereby decreasing the transcription of lipogenic genes in cells.[45] More studies are required regarding the efficacy of this potential target in reducing circulating LDL-C since it also induces the expression of PCSK9 - a serine protease which promotes degradation of LDLR, thereby preventing the clearing of LDL particles from the plasma.

Table

Class Drug Company Agent Name Mechanism of Action Efficacy on Lowering LDL-C Route of Administration Adverse Effects Published Clinical Trials
Inhibition of Apo B/Antisense oligonucleotides ISIS Pharmaceuticals ISIS-301012 or Mipomersen Inhibits apo B mRNA gene expression Up to 50% reduction Subcutaneous injection (SC) Injection site reactions, flu-like illness, 3-fold asymptomatic elevation of liver transaminases I, II, III
PCSK9 Inhibition
MTP Inhibition Aegerion Pharmaceuticals, Pfizer, Surface Logix Intestinal non-specific (lometapide, implitapide, CP-34086); Intestinal-specific (SLx-4090, dirlotapide, JTT-130) Inhibits Microsomal triglyceride transfer protein Lometapide (up to 50%), CP-34086 (up to 70%) PO Intestinal non-specific agents causes GI adverse effects, increases in hepatic fat Lometapide (I, II, III), JTT-130 (I, II)
Thyromimetics
Squalene Synthase Inhibitors

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