Delving into the Latest Updates on Anacetrapib with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Anacetrapib (JAN/USAN)

Target

CETP

Mechanism

CETP inhibitors(Cholesteryl ester transfer protein inhibitors)

Therapeutic Areas

Cardiovascular DiseasesCongenital DisordersEndocrinology and Metabolic Disease+ [1]

Active Indication-

Inactive Indication

AtherosclerosisCoronary DiseaseDyslipidemias+ [9]

Originator Organization

Merck Sharp & Dohme Corp.

Active Organization-

Inactive Organization

Merck Sharp & Dohme Corp.Merck Sharp & Dohme LLC

Drug Highest PhaseDiscontinuedPhase 3

First Approval Date-

RegulationSpecial Review Project (CN)

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Structure/Sequence

Molecular FormulaC30H25F10NO3

InChIKeyMZZLGJHLQGUVPN-HAWMADMCSA-N

CAS Registry875446-37-0

There are currently no studies evaluating the effect of anacetrapib on blood vessel function and stiffness of the arteries. The REVEAL-Vasc trial will assess whether anacetrapib, in addition to atorvastatin (LDL-C lowering drug) treatment, results in greater endothelial-dependent vascular function and aortic stiffness in patients with established cardiovascular disease, compared to adding placebo.
Participants will be asked to provide a blood sample and pulse Wave Velocity/Pulse Wave Analysis and Flow Mediated Dilation will be carried out to assess blood vessel function and stiffness of the arteries. REVEAL-Vasc is an investigator led sub-study of HPS3/TIMI 55: REVEAL (Randomized Evaluation of the Effects of Anacetrapib through Lipid modification): A large-scale, randomized placebo-controlled trial of the clinical effects of anacetrapib among people with established vascular disease (NCT01252953) which is coordinated by OXFORD CTSU.
No treatment will be received on this sub-study, therefore only participants who have been enrolled in HPS3/TIMI55 REVEAL in which participants received anacetrapib with atorvastatin or placebo will be considered for this trial.

Start Date01 Jan 2017

Sponsor / Collaborator

Cambridge University Hospitals NHS Foundation Trust

CTR20130983

/ CompletedNot Applicable

在中国健康受试者中进行的MK-0859单次给药和多次给药的药代动力学研究

[Translation] Single-dose and multiple-dose pharmacokinetic study of MK-0859 in healthy Chinese subjects

评估50-、 100-、200-mg MK-0859在中国患者中药代动力学特征

[Translation]

To evaluate the pharmacokinetic characteristics of 50-, 100-, and 200-mg MK-0859 in Chinese patients

Start Date30 May 2016

Sponsor / Collaborator

Merck Sharp & Dohme (China) Ltd.

[+1]

PER-004-14

/ Unknown statusPhase 3

A WORLDWIDE, MULTICENTER, DOUBLE-BLIND, RANDOMIZED, PLACEBO-CONTROLLED STUDY TO ASSESS THE TOLERABILITY AND EFFICACY OF ANACETRAPIB WHEN ADDED TO ONGOING THERAPY WITH A STATIN IN PATIENTS WITH CORONARY HEART DISEASE (CHD) OR CHD RISK-EQUIVALENT DISEASE: EVALUATION OF ANACETRAPIB LEVELS IN PLASMA AND ADIPOSE TISSUE IN PATIENTS WHO WERE PREVIOUSLY TREATED WITH ANACETRAPIB IN THE PROTOCOL 019, DEFINE STUDY

Start Date14 May 2014

Sponsor / Collaborator-

100 Clinical Results associated with Anacetrapib

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100 Translational Medicine associated with Anacetrapib

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100 Patents (Medical) associated with Anacetrapib

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226

Literatures (Medical) associated with Anacetrapib

01 Dec 2024·Pharmacology Research & Perspectives

Obicetrapib exhibits favorable physiochemical and pharmacokinetic properties compared to previous cholesteryl ester transfer protein inhibitors: An integrated summary of results from non‐human primate studies and clinical trials

Review

Author: Kling, Douglas ; Kastelein, John J. P. ; Curcio, Danielle ; Davidson, Michael H. ; Nicholls, Stephen J. ; Ditmarsch, Marc ; Hsieh, Andrew ; Nelson, Adam J. ; Johnson, Judith ; Kirkpatrick, Carol F.

AbstractAnacetrapib, a cholesteryl ester transfer protein (CETP) inhibitor previously under development, exhibited an usually extended terminal half‐life and large food effect and accumulated in adipose tissue. Other CETP inhibitors have not shown such effects. Obicetrapib, a potent selective CETP inhibitor, is undergoing Phase III clinical development. Dedicated assessments were conducted in pre‐clinical and Phase I and II clinical studies of obicetrapib to examine the pharmacokinetic issues observed with anacetrapib. After 9 months of dosing up to 50 mg/kg/day in cynomolgus monkeys, obicetrapib was completely eliminated from systemic circulation and not detected in adipose tissue after a 13‐week recovery period. In healthy humans receiving 1–25 mg of obicetrapib, the mean terminal half‐life of obicetrapib was 148, 131, and 121 h at 5, 10, and 25 mg, respectively, and food increased plasma levels by ~1.6‐fold with a 10 mg dose. At the end of treatment in Phase II trials, mean plasma levels of obicetrapib ranged from 194.5 ng/mL with 2.5 mg to 506.3 ng/mL with 10 mg. Plasma levels of obicetrapib decreased by 92.2% and 98.5% at four and 15 weeks post‐treatment, respectively. Obicetrapib shows no clinically relevant accumulation, is minimally affected by food, and has a mean terminal half‐life of 131 h for the 10 mg dose. These data support once daily, chronic dosing of obicetrapib in Phase III trials for dyslipidemia management.

01 Nov 2024·Food Science & Nutrition

Assessing lipid‐lowering and plasma cholesteryl ester transfer protein activity of Centranthus longiflorus and β‐Sitosterol following administration to triton WR1339‐ treated rats

Article

Author: Umudum, Fatma Zuhal ; Askin, Seda

AbstractThe aim of this study was to evaluate the lipid‐lowering and plasma cholesteryl ester transfer protein(CETP) activity of Centranthus longiflorus(CL) and β‐Sitosterol(βS) following intraperitoneal administration of Triton‐WR 1339 (=Tyloxapol) (TWR) to male Wistar rats. Hyperlipidemia(HL) was developed by intraperitoneal injection of TWR. The animals were divided into main eight groups of six rats each. Rats were housed in separate cages and fed a standard diet for 7 days. After 7 days, ethanol extraction of CL plant, aqueous suspension of βS and anacetrapib was given to rats by oral gavage 1 h before the triton injection. Blood samples were collected and used for the biochemical parameters analysis. Histopathological studies were also performed on liver tissue. In hyperlipidemic rats(HR), CL extract and βS reduced total cholesterol similarly. βS lowered low‐density lipoprotein(LDL‐C) more than CL extract. Both CL extract and βS approximated impaired Alanine transaminase(ALT) and Aspartate transaminase(AST) levels in HR's to the level of control. CL extract provided better protection than βS against deterioration in liver tissue samples seen in hyperlipidemic rats. Finally, CL extract and βS inhibited CETP, at which point βS was more effective. These findings showed that CL extract and βS reduce plasma lipid concentration and may have a hypolipidemic effect due to their anti‐CETP properties.

17 Aug 2024·Bioanalysis

Quantitation of anacetrapib in human and animal adipose by liquid chromatography with mass spectrometric detection

Article

Author: Roadcap, Brad ; Lutz, Ryan W ; Li, Hankun ; Schlegel, Jessica ; Woolf, Eric ; Schiller, James ; Chavez-Eng, Cynthia M ; Fang, Wei

Cholesteryl ester transfer protein (CETP) inhibitor is a target for both lowering low-density lipoproteins and raising high-density lipoproteins. Anacetrapib was the lead compound in our cholesteryl ester transfer protein inhibitor program. Preclinical studies were initiated to support the safety of anacetrapib deposition in adipose tissue, followed by a clinical trial to evaluate the effects of anacetrapib in people with vascular disease. An ultra-high performance liquid chromatography/tandem mass spectrometry method was developed to determine tissue anacetrapib concentrations in the adipose of three animal species and humans. The assays were validated in the concentration ranges of 5-5000 ng/ml and 0.1-100 μg/ml. The anacetrapib concentrations in adipose tissue from preclinical and clinical studies were determined.

1

News (Medical) associated with Anacetrapib

14 Jan 2021

·www.biospace.com

NewAmsterdam Pharma Completes $196M (€160M) Series A Funding for Comprehensive Phase 3 Development Program

Jan. 14, 2021 11:00 UTC Founding investor Forbion joined by co-lead investors, Morningside Ventures and Ascendant BioCapital, and other leaders in global biopharmaceutical investment Funding will support initiation and finalization of Phase 3 development of obicetrapib, a potent ApoB and LDL-c lowering small molecule drug, intended for patients not well-controlled on statins NewAmsterdam Pharma welcomes Jason Dinges of Morningside and Gaurav Gupta, MD of Ascendant BioCapital to its board of directors NAARDEN, the Netherlands--(BUSINESS WIRE)-- NewAmsterdam Pharma (NAP), a clinical stage company focused on the research and development of transformative therapies for cardio-metabolic diseases, today announced completion of a $196M (€160M) Series A funding round. The financing will support the full Phase 3 development of its ApoB and LDL-c lowering small molecule drug, obicetrapib. The drug, a cholesteryl ester transfer protein (CETP) inhibitor, is being developed for patients who are not well-controlled on statins. Forbion, NAP’s founding investor, was joined by Morningside Ventures and Ascendant BioCapital as co-lead investors in the Series A financing. Also participating in this funding round were Kaiser Foundation Hospitals, BVF Partners L.P., Population Health Partners, LSP Dementia Fund, Peter Thiel, Janus Henderson Investors, Medpace, GL Capital, JVC Investment Partners, and Presight Capital. “This is an important milestone in the advancement of obicetrapib and the growth of NewAmsterdam Pharma,” said Michael Davidson, MD, chief executive officer of NewAmsterdam Pharma. “The tremendous support of our investors allows us to initiate a large, Phase 3 development program as we work to create a new option for the millions of high cardiovascular risks patients globally who, despite maximally tolerated statin therapy, require additional LDL-c lowering options.” “Effectively inhibiting CETP to reduce atherosclerotic risk in patients is something Dr. Davidson and I have been endeavoring to achieve in our field of research for more than two decades,” said John Kastelein, MD, PhD, FESC, chief scientific officer of NewAmsterdam Pharma. “Long term follow up from the 2017 REVEAL study validated CETP as a target to lower LDL-c and reduce major adverse cardiac events (MACE).1 We believe that in obicetrapib, based on clinical studies to date, we have a molecule which is well tolerated and has not shown any of the safety issues of previous CETP inhibitors. Furthermore, based on the surrogate endpoints of the REVEAL study, obicetrapib was shown to be more effective at lowering LDL-c at a 5 mg dose in comparison to a 100 mg dose of anacetrapib.” “We are very pleased to support the development of obicetrapib and contribute to the success of NAP,” said Jason Dinges of Morningside. “We believe that obicetrapib has a unique efficacy and safety pro will further demonstrate not only a potent LDL-c lowering ability but other key attributes which could potentially benefit the large and underserved number of patients at risk of cardiovascular disease. We have confidence in the deep expertise and proven track record of Dr. Davidson and Dr. Kastelein to deliver these results.” “Cardiovascular disease remains the leading cause of disability-adjusted life years globally, and tens of millions of patients struggle to reach LDL-c goals on current therapies, demonstrating a clear need for novel agents,” said Gaurav Gupta, MD of Ascendant BioCapital. “CETP-silencing mutations correspond to lower cardiovascular risk, and given the potent pharmacology demonstrated in the TULIP study2, we expect obicetrapib to become a significant part of the treatment paradigm for dyslipidemia globally.” Two Phase 2b clinical trials for obicetrapib are underway with targeted completion in Q2 2021. NAP is looking to initiate Phase 3 clinical trials in Q4 2021. About Obicetrapib Obicetrapib is a cholesteryl ester transfer protein (CETP) inhibitor which targets Apolipoprotein B (ApoB) and low-density lipoprotein cholesterol (LDL-c) in the body. Millions of people globally have cannot achieve LDL-c goals despite maximally tolerated statin therapy.3 A Phase 2b study called TULIP, published in The Lancet, showed that obicetrapib significantly reduced the number of ApoB-containing particles that constitute LDL-c and was well tolerated in patients with mild dyslipidemia. The randomized, double-blind, placebo-controlled study tested the drug in 364 patients, to assess the safety, tolerability, and efficacy of the potential therapy. Two Phase 2b clinical trials for obicetrapib are underway with targeted completion in Q2 2021. NAP is working to initiate Phase 3 trials in Q4 2021. About NewAmsterdam Pharma Founded in 2019 by the venture capital firm Forbion and John Kastelein, NewAmsterdam Pharma is a privately held, clinical-stage company focused on the research and development of transformative therapies for cardiometabolic diseases. Its mission is to improve patient care in populations where traditional therapies are not tolerated or have been unsuccessful. In April 2020, NewAmsterdam acquired Dezima Pharma from Amgen, including all rights for obicetrapib (formerly AMG 899, now TA-8995) a selective cholesteryl ester transfer protein (CETP) inhibitor. The Company is investigating obicetrapib as the preferred ApoB and LDL-c lowering therapy for patients with ASCVD/FH on the maximally tolerated dose of statin therapy. NewAmsterdam Pharma is headquartered in Naarden, The Netherlands. For more information, please visit: 1 2 Hovingh GK, Kastelein JP, van Deventer SJH, Round P, Ford, J, Saleheen D, et. al. Cholesterol ester transfer protein inhibition by TA-8995 in patients with mild dyslipidemia (TULIP): a randomized, double-blind, placebo-controlled phase 2 trial. The Lancet 2015.386(9992): 452-460. DOI: (15)60158-1 3 Ray K et al. EU-Wide Cross-Sectional Observational Study of Lipid-Modifying Therapy Use in Secondary and Primary Care: the DAVINCI study, European Journal of Preventive Cardiology 2020 View source version on businesswire.com: Contacts Media and Investor Inquiries: NewAmsterdam Pharma McDougall Communications on behalf of New Amsterdam Pharma Elizabeth Harness, P: +1 585-435-7379, elizabeth@mcdougallpr.com Christopher Knospe, P: +1 716-440-5580, chris@mcdougallpr.com Source: NewAmsterdam Pharma View this news release online at:

Small molecular drug

100 Deals associated with Anacetrapib

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External Link

KEGG	Wiki	ATC	Drug Bank
D08855	Anacetrapib	-	DB06630

R&D Status

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Atherosclerosis	Phase 3	GB	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	DE	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	GB	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	IT	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	US	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	SE	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	NO	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	CN	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	DK	Merck Sharp & Dohme Corp.	31 May 2006
Myocardial Infarction	Phase 3	FI	Merck Sharp & Dohme Corp.	31 May 2006

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Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT01524289 (REALIZE \| 0859-020 \| MK-0859-020, CTgov)	Phase 3	Heterozygous familial hypercholesterolemia \| Hyperlipoproteinemia Type II	306	Placebo	qbincuxyqm(ylzdaygkmk) = gqdskbnvyz nxbfbvsgmm (rqwykhkzgg, jjechypihz - aifmnhnsbc) View more	-	28 Aug 2019
NCT01252953 (REVEAL, CTgov)	Phase 3	Atherosclerosis	30,449	Anacetrapib (Anacetrapib)	sajkglpqhl(oemctewgyg) = qsitlurmyk dnemgqccaz (vubuuzxuiq, dbizmwyjkh - afbyjutwrd) View more	-	04 May 2018
				Placebo anacetrapib (Placebo Anacetrapib)	sajkglpqhl(oemctewgyg) = wfjwnwfvlh dnemgqccaz (vubuuzxuiq, bkzncnwjvn - xpcdfvpdwe) View more
NCT01252953 (REVEAL, Pubmed \| Br Dent J \| N Engl J Med) Manual	Phase 3	Atherosclerosis	30,449	Anacetrapib	wmryehjhah(wnjknkczfn) = osxqnvyahh pvzwdotlrb (lonlhjfukq )	Positive	28 Sep 2017
				Placebo	wmryehjhah(wnjknkczfn) = ceicpwvikc pvzwdotlrb (lonlhjfukq )
NCT00990808 (0859-026, Pubmed \| Arterioscler Thromb Vasc Biol)	Phase 1	Hypercholesterolemia	39	Anacetrapib	mucceagmoo(fsnrublbqv) = ycfabbtpbi zhbadcqyrg (psfbzyildh )	-	01 Sep 2017
NCT01524289 (ESC2017)	Phase 3	Heterozygous familial hypercholesterolemia LDLR \| APOB \| PCSK9	306	Anacetrapib 100 mg	(sqzdfoaipq) = beisiflvbf dqanaueycm (iozzmjzlrd )	-	26 Aug 2017
NCT01860729 (MK-0859-022, Pubmed \| Am J Cardiol) Manual	Phase 3	Hypercholesterolemia	583	ongoing therapy with statin ± other lipid-modifying therapies+Anacetrapib	klhqgyxxnf(hbfxcimadb) = There were no clinically meaningful differences between the anacetrapib and placebo groups in the % patients who discontinued drug due to an adverse event or in abnormalities in liver enzymes, creatine kinase, blood pressure, electrolytes, or adjudicated cardiovascular events. wbjnssxhbd (euocgzykfg ) View more	Positive	15 Aug 2017
				ongoing therapy with statin ± other lipid-modifying therapies+Placebo
NCT01760460 (Pubmed \| Atherosclerosis) Manual	Phase 3	Dyslipidemias	307	anacetrapib	(tpzvnukdxq) = ijcclaaozo gkohiluarb (hsepntwvti ) View more	Positive	01 Jun 2017
				Placebo	-
NCT01824238 (Pubmed \| Atherosclerosis) Manual	Phase 3	Heterozygous familial hypercholesterolemia	68	anacetrapib	(whqfzwdjgw) = There were no differences between the groups in the proportion of patients who discontinued drug due to an adverse event or abnormalities in liver enzymes, creatinine kinase, blood pressure, electrolytes or adjudicated cardiovascular events. hfzhvtyiyd (yiqejmluev ) View more	Positive	01 Jun 2016
				Placebo
NCT01524289 (REALIZE, Pubmed \| Lancet) Manual	Phase 3	Heterozygous familial hypercholesterolemia	306	Anacetrapib	(ftaiitoase) = qwmtcwplpu ozhidlnwzl (lyebdabzco ) View more	Positive	30 May 2015
				Placebo	(ftaiitoase) = pqfiswybyq ozhidlnwzl (lyebdabzco ) View more
NCT00685776 (0859-019 \| DEFINE, Pubmed \| J Clin Lipidol) Manual	Phase 3	Coronary Disease	-	Anacetrapib	(blsqyhpano) = xzqofrqydu waaaqqoevo (theiyvquar ) View more	Similar	01 Jan 2015