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An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes

Proprotein convertase subtilisin/kexin type 9 (PCSK9) is a promising therapeutic target for treating coronary heart disease. We report a novel antibody 1B20 that binds to PCSK9 with sub-nanomolar affinity and antagonizes PCSK9 function in-vitro. In CETP/LDLR-hemi mice two successive doses of 1B20, a...

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Autores principales: Zhang, Liwen, McCabe, Timothy, Condra, Jon H., Ni, Yan G., Peterson, Laurence B., Wang, Weirong, Strack, Alison M., Wang, Fubao, Pandit, Shilpa, Hammond, Holly, Wood, Dana, Lewis, Dale, Rosa, Ray, Mendoza, Vivienne, Cumiskey, Anne Marie, Johns, Douglas G., Hansen, Barbara C., Shen, Xun, Geoghagen, Neil, Jensen, Kristian, Zhu, Lei, Wietecha, Karol, Wisniewski, Douglas, Huang, Lingyi, Zhao, Jing Zhang, Ernst, Robin, Hampton, Richard, Haytko, Peter, Ansbro, Frances, Chilewski, Shannon, Chin, Jayne, Mitnaul, Lyndon J., Pellacani, Andrea, Sparrow, Carl P., An, Zhiqiang, Strohl, William, Hubbard, Brian, Plump, Andrew S., Blom, Daniel, Sitlani, Ayesha
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3282994/
https://www.ncbi.nlm.nih.gov/pubmed/22355267
http://dx.doi.org/10.7150/ijbs.3524
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author Zhang, Liwen
McCabe, Timothy
Condra, Jon H.
Ni, Yan G.
Peterson, Laurence B.
Wang, Weirong
Strack, Alison M.
Wang, Fubao
Pandit, Shilpa
Hammond, Holly
Wood, Dana
Lewis, Dale
Rosa, Ray
Mendoza, Vivienne
Cumiskey, Anne Marie
Johns, Douglas G.
Hansen, Barbara C.
Shen, Xun
Geoghagen, Neil
Jensen, Kristian
Zhu, Lei
Wietecha, Karol
Wisniewski, Douglas
Huang, Lingyi
Zhao, Jing Zhang
Ernst, Robin
Hampton, Richard
Haytko, Peter
Ansbro, Frances
Chilewski, Shannon
Chin, Jayne
Mitnaul, Lyndon J.
Pellacani, Andrea
Sparrow, Carl P.
An, Zhiqiang
Strohl, William
Hubbard, Brian
Plump, Andrew S.
Blom, Daniel
Sitlani, Ayesha
author_facet Zhang, Liwen
McCabe, Timothy
Condra, Jon H.
Ni, Yan G.
Peterson, Laurence B.
Wang, Weirong
Strack, Alison M.
Wang, Fubao
Pandit, Shilpa
Hammond, Holly
Wood, Dana
Lewis, Dale
Rosa, Ray
Mendoza, Vivienne
Cumiskey, Anne Marie
Johns, Douglas G.
Hansen, Barbara C.
Shen, Xun
Geoghagen, Neil
Jensen, Kristian
Zhu, Lei
Wietecha, Karol
Wisniewski, Douglas
Huang, Lingyi
Zhao, Jing Zhang
Ernst, Robin
Hampton, Richard
Haytko, Peter
Ansbro, Frances
Chilewski, Shannon
Chin, Jayne
Mitnaul, Lyndon J.
Pellacani, Andrea
Sparrow, Carl P.
An, Zhiqiang
Strohl, William
Hubbard, Brian
Plump, Andrew S.
Blom, Daniel
Sitlani, Ayesha
author_sort Zhang, Liwen
collection PubMed
description Proprotein convertase subtilisin/kexin type 9 (PCSK9) is a promising therapeutic target for treating coronary heart disease. We report a novel antibody 1B20 that binds to PCSK9 with sub-nanomolar affinity and antagonizes PCSK9 function in-vitro. In CETP/LDLR-hemi mice two successive doses of 1B20, administered 14 days apart at 3 or 10 mpk, induced dose dependent reductions in LDL-cholesterol (≥ 25% for 7-14 days) that correlated well with the extent of PCSK9 occupancy by the antibody. In addition, 1B20 induces increases in total plasma antibody-bound PCSK9 levels and decreases in liver mRNA levels of SREBP-regulated genes PCSK9 and LDLR, with a time course that parallels decreases in plasma LDL-cholesterol (LDL-C). Consistent with this observation in mice, in statin-responsive human primary hepatocytes, 1B20 lowers PCSK9 and LDLR mRNA levels and raises serum steady-state levels of antibody-bound PCSK9. In addition, mRNA levels of several SREBP regulated genes involved in cholesterol and fatty-acid synthesis including ACSS2, FDPS, IDI1, MVD, HMGCR, and CYP51A1 were decreased significantly with antibody treatment of primary human hepatocytes. In rhesus monkeys, subcutaneous (SC) dosing of 1B20 dose-dependently induces robust LDL-C lowering (maximal ~70%), which is correlated with increases in target engagement and total antibody-bound PCSK9 levels. Importantly, a combination of 1B20 and Simvastatin in dyslipidemic rhesus monkeys reduced LDL-C more than either agent alone, consistent with a mechanism of action that predicts additive effects of anti-PCSK9 agents with statins. Our results suggest that antibodies targeting PCSK9 could provide patients powerful LDL lowering efficacy on top of statins, and lower cardiovascular risk.
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spelling pubmed-32829942012-02-21 An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes Zhang, Liwen McCabe, Timothy Condra, Jon H. Ni, Yan G. Peterson, Laurence B. Wang, Weirong Strack, Alison M. Wang, Fubao Pandit, Shilpa Hammond, Holly Wood, Dana Lewis, Dale Rosa, Ray Mendoza, Vivienne Cumiskey, Anne Marie Johns, Douglas G. Hansen, Barbara C. Shen, Xun Geoghagen, Neil Jensen, Kristian Zhu, Lei Wietecha, Karol Wisniewski, Douglas Huang, Lingyi Zhao, Jing Zhang Ernst, Robin Hampton, Richard Haytko, Peter Ansbro, Frances Chilewski, Shannon Chin, Jayne Mitnaul, Lyndon J. Pellacani, Andrea Sparrow, Carl P. An, Zhiqiang Strohl, William Hubbard, Brian Plump, Andrew S. Blom, Daniel Sitlani, Ayesha Int J Biol Sci Research Paper Proprotein convertase subtilisin/kexin type 9 (PCSK9) is a promising therapeutic target for treating coronary heart disease. We report a novel antibody 1B20 that binds to PCSK9 with sub-nanomolar affinity and antagonizes PCSK9 function in-vitro. In CETP/LDLR-hemi mice two successive doses of 1B20, administered 14 days apart at 3 or 10 mpk, induced dose dependent reductions in LDL-cholesterol (≥ 25% for 7-14 days) that correlated well with the extent of PCSK9 occupancy by the antibody. In addition, 1B20 induces increases in total plasma antibody-bound PCSK9 levels and decreases in liver mRNA levels of SREBP-regulated genes PCSK9 and LDLR, with a time course that parallels decreases in plasma LDL-cholesterol (LDL-C). Consistent with this observation in mice, in statin-responsive human primary hepatocytes, 1B20 lowers PCSK9 and LDLR mRNA levels and raises serum steady-state levels of antibody-bound PCSK9. In addition, mRNA levels of several SREBP regulated genes involved in cholesterol and fatty-acid synthesis including ACSS2, FDPS, IDI1, MVD, HMGCR, and CYP51A1 were decreased significantly with antibody treatment of primary human hepatocytes. In rhesus monkeys, subcutaneous (SC) dosing of 1B20 dose-dependently induces robust LDL-C lowering (maximal ~70%), which is correlated with increases in target engagement and total antibody-bound PCSK9 levels. Importantly, a combination of 1B20 and Simvastatin in dyslipidemic rhesus monkeys reduced LDL-C more than either agent alone, consistent with a mechanism of action that predicts additive effects of anti-PCSK9 agents with statins. Our results suggest that antibodies targeting PCSK9 could provide patients powerful LDL lowering efficacy on top of statins, and lower cardiovascular risk. Ivyspring International Publisher 2012-02-09 /pmc/articles/PMC3282994/ /pubmed/22355267 http://dx.doi.org/10.7150/ijbs.3524 Text en © Ivyspring International Publisher. This is an open-access article distributed under the terms of the Creative Commons License (http://creativecommons.org/licenses/by-nc-nd/3.0/). Reproduction is permitted for personal, noncommercial use, provided that the article is in whole, unmodified, and properly cited.
spellingShingle Research Paper
Zhang, Liwen
McCabe, Timothy
Condra, Jon H.
Ni, Yan G.
Peterson, Laurence B.
Wang, Weirong
Strack, Alison M.
Wang, Fubao
Pandit, Shilpa
Hammond, Holly
Wood, Dana
Lewis, Dale
Rosa, Ray
Mendoza, Vivienne
Cumiskey, Anne Marie
Johns, Douglas G.
Hansen, Barbara C.
Shen, Xun
Geoghagen, Neil
Jensen, Kristian
Zhu, Lei
Wietecha, Karol
Wisniewski, Douglas
Huang, Lingyi
Zhao, Jing Zhang
Ernst, Robin
Hampton, Richard
Haytko, Peter
Ansbro, Frances
Chilewski, Shannon
Chin, Jayne
Mitnaul, Lyndon J.
Pellacani, Andrea
Sparrow, Carl P.
An, Zhiqiang
Strohl, William
Hubbard, Brian
Plump, Andrew S.
Blom, Daniel
Sitlani, Ayesha
An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes
title An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes
title_full An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes
title_fullStr An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes
title_full_unstemmed An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes
title_short An Anti-PCSK9 Antibody Reduces LDL-Cholesterol On Top Of A Statin And Suppresses Hepatocyte SREBP-Regulated Genes
title_sort anti-pcsk9 antibody reduces ldl-cholesterol on top of a statin and suppresses hepatocyte srebp-regulated genes
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3282994/
https://www.ncbi.nlm.nih.gov/pubmed/22355267
http://dx.doi.org/10.7150/ijbs.3524
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