Orally Bioavailable Macrocyclic Peptide That Inhibits Binding of PCSK9 to the Low Density Lipoprotein Receptor

Johns, Douglas G.; Campeau, Louis‐Charles; Banka, Puja; Bautmans, An; Bueters, Tjerk; Bianchi, Elisabetta; Branca, Danila; Bulger, Paul G.; Crèvecoeur, Inne; Ding, Fa‐Xiang; Garbaccio, R. M.; Guetschow, Erik; Guo, Yan; Ha, Sookhee; Johnston, Jennifer M.; Josien, Hubert; Kauh, Eunkyung A; Koeplinger, Kenneth A.; Kuethe, Jeffrey T.; Lai, Eseng; Lanning, Christine L; Lee, Anita Y. H.; Li, Li; Nair, Anilkumar G.; O’Neill, Edward A.; Stoch, S Aubrey; Thaisrivongs, David A.; Tucker, Thomas J.; Váchal, Petr; Dyck, Kristien Van; Vanhoutte, Frederic P; Volckaert, Bram; Wolford, Dennis; Xu, Y.; Zhang, Tian; Zhou, Dan; Zhou, Hong; Zhu, Xiaoyan; Zokian, Hratch; Walji, Abbas M.; Wood, Harold B.

doi:10.1161/circulationaha.122.063372

Cited by 36 publications

(30 citation statements)

References 34 publications

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“…15 The cyclic peptide MK-0616 may present an alternative to currently available PCSK9 inhibitors, especially for patients who prefer oral medications or who cannot access the subcutaneous formulations. In the study by Johns et al, 11 MK-0616 demonstrated the ability to effectively decrease LDL-C levels, both as monotherapy and in combination with statin treatment. According to the data on other PCSK9 inhibitors, it is likely that MK-0616 will also prove to be effective in preventing cardiovascular disease and reducing the incidence of adverse cardiovascular events.…”

Section: Article See P 144mentioning

confidence: 99%

“…Furthermore, 2 phase 1 studies were performed to evaluate the pharmacodynamics and safety profile of MK-0616 in humans. 11 In the first study, 60 healthy male volunteers received a single-ascending dose of the drug, whereas the second study tested a multiple-risingdose regimen in statin-treated patients. In the first study, participants were given a single dose during a specific period.…”

Section: Article See P 144mentioning

confidence: 99%

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New Chapter in the PCSK9 Book: Oral Inhibition of PCSK9 Binding to the LDL Receptor With a Macrocyclic Peptide

Landmesser

Makhmudova

2023

Circulation

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Section: Article See P 144mentioning

confidence: 99%

Section: Article See P 144mentioning

confidence: 99%

New Chapter in the PCSK9 Book: Oral Inhibition of PCSK9 Binding to the LDL Receptor With a Macrocyclic Peptide

Landmesser

Makhmudova

2023

Circulation

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“…17 In turn, Merck recently disclosed the structure of MK-0616, an oral proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitor, which in a recent Phase 2b study, significantly reduced LDL-C in patients with hypercholesterolemia. 18 Potency and protease stability were obtained through introduction of a fluorinated tryptophan, D-Ala (AA2), α-Me-Pro (AA8), and cross-linking, ultimately yielding an oral MP inhibitor at a fraction of the size of current monoclonal antibody injectables.…”

mentioning

confidence: 99%

“…For Chugai, their first clinical macrocyclic peptide for intracellular rat sarcoma virus (RAS) inhibition was identified through incorporation of multiple N -substituted ncAAs, reducing the polar surface area and improving membrane permeability . In turn, Merck recently disclosed the structure of MK-0616, an oral proprotein convertase subtilisin/kexin type 9 (PCSK9) inhibitor, which in a recent Phase 2b study, significantly reduced LDL-C in patients with hypercholesterolemia . Potency and protease stability were obtained through introduction of a fluorinated tryptophan, d -Ala (AA2), α-Me-Pro (AA8), and cross-linking, ultimately yielding an oral MP inhibitor at a fraction of the size of current monoclonal antibody injectables.…”

mentioning

confidence: 99%

Beyond 20 in the 21st Century: Prospects and Challenges of Non-canonical Amino Acids in Peptide Drug Discovery

Hickey

Sindhikara

Zultanski

et al. 2023

ACS Med. Chem. Lett.

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Life is constructed primarily using a toolbox of 20 canonical amino acids�relying upon these building blocks for the assembly of proteins and peptides that regulate nearly every cellular task, including cell structure, function, and maintenance. While Nature continues to be a source of inspiration for drug discovery, medicinal chemists are not beholden to only 20 canonical amino acids and have begun to explore non-canonical amino acids (ncAAs) for the construction of designer peptides with improved drug-like properties. However, as our toolbox of ncAAs expands, drug hunters are encountering new challenges in approaching the iterative peptide design−make−test−analyze cycle with a seemingly boundless set of building blocks. This Microperspective focuses on new technologies that are accelerating ncAA interrogation in peptide drug discovery (including HELM notation, late-stage functionalization, and biocatalysis) while shedding light on areas where further investment could not only accelerate the discovery of new medicines but also improve downstream development.

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“…An error has been identified in Figure regarding the structure and caption of MK-0616 ( 5 ). The functional group on the terminal aryl is incorrectly depicted as −OH; the correct functional group is −OCH 3 on the terminal aryl ring. , The corrected Figure is shown below:…”

mentioning

confidence: 99%

Correction to “Recent Update on the Development of PCSK9 Inhibitors for Hypercholesterolemia Treatment”

Ahamad¹,

Bhat²

2023

J. Med. Chem.

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show abstract

Orally Bioavailable Macrocyclic Peptide That Inhibits Binding of PCSK9 to the Low Density Lipoprotein Receptor

Cited by 36 publications

References 34 publications

New Chapter in the PCSK9 Book: Oral Inhibition of PCSK9 Binding to the LDL Receptor With a Macrocyclic Peptide

New Chapter in the PCSK9 Book: Oral Inhibition of PCSK9 Binding to the LDL Receptor With a Macrocyclic Peptide

Beyond 20 in the 21st Century: Prospects and Challenges of Non-canonical Amino Acids in Peptide Drug Discovery

Correction to “Recent Update on the Development of PCSK9 Inhibitors for Hypercholesterolemia Treatment”

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