Serum Proteomic Analysis of Peripartum Cardiomyopathy Reveals Distinctive Dysregulation of Inflammatory and Cholesterol Metabolism Pathways

围产期心肌病 下调和上调 内科学 心肌病 病理生理学 炎症 生物途径 内分泌学 医学 视黄醇X受体 心力衰竭 生物 转录因子 核受体 基因表达 基因 遗传学
作者
Jana Lovell,Kevin C. Bermea,Jinsheng Yu,Sylvie Rousseau,Charles D. Cohen,Aashik Bhalodia,Marcelle Dina Zita,Richard D. Head,Roger S. Blumenthal,Rami Alharethi,Julie B. Damp,John Boehmer,Jeffrey D. Alexis,Dennis M. McNamara,Garima Sharma,Luigi Adamo,Dennis M. aaaMcNamara,James D. Fett,Jessica Pisarcik,Charles F. McTiernan,Karen Hanley-Yanez,John Gorcsan,Erik B. Schelbert,Rami Alharethi,Kismet Rasmusson,Kim Brunisholz,Amy L. Butler,D. Budge,Abdallah G. Kfoury,Benjamin D. Horne,Joe Tuinei,Heather Brown,Julie B. Damp,Allen J. Naftilan,Jill Russell,Darla Freehardt,Eileen Hsich,Cynthia Oblak,Greg Ewald,Donna Whitehead,Jean Flanagan,Anne Platts,Uri Elkayam,Jorge Caro,Stephanie Mullin,Michael M. Givertz,Mary Susan Anello,Navin Rajagopalan,David R. Booth,Tiffany Sandlin,Wendy Wijesiri,Leslie T. Cooper,Lori A. Blauwet,Joann Brunner,Mary Phelps,Ruth Kempf,Kalgi Modi,Tracy Norwood,Joan Briller,Decebal Sorin Griza,G. Michael Felker,Robb D. Kociol,Patricia L. Adams,Gretchen Wells,Vinay Thohan,Deborah Wesley‐Farrington,Sandra Soots,Richard Sheppard,Caroline Michel,Nathalie Lapointe,Heather Nathaniel,Angela Kealey,Marc J. Semigran,Maureen Daher,John Boehmer,David Silber,Eric Popjes,Patricia Frey,Todd Nicklas,Jeffrey D. Alexis,Lori Caufield,John W. Thornton,Mindy Gentry,V.J. Robinson,Gyanendra K. Sharma,Joan Holloway,Maria Powell,David W. Markham,Mark H. Drazner,Lynn Fernandez,Mark Zucker,David A. Baran,Martin L. Gimovsky,Natalia Hochbaum,Bharati Patel,Laura L. Adams,Gautam Ramani,Stephen S. Gottlieb,Shawn Robinson,Stacy D. Fisher,Joanne Marshall,Jennifer Haythe,Donna Mancini,Rachel Bijou,Maryjane Farr,Marybeth Marks,Henry Arango,Biykem Bozkurt,Mariana Bolos,Paul Mather,Sharon Rubin,Raphael Bonita,Susan Eberwine,Hal A. Skopicki,Kathleen Stergiopoulos,Ellen McCathy-Santoro,Jennifer Intravaia,Elizabeth W. Maas,Jordan Safirstein,Audrey Kleet,Nancy Martinez,Christine Corpoin,Donna Hesari,Sandra Chaparro,Laura J. Hudson,Jalal K. Ghali,Zora Injic,Ilan S. Wittstein,Dennis M. McNamara,Karen Janosko,Charles F. McTiernan,Barry London,Karen Hanley-Yanez,John Gorcsan,Hidekazu Tanaka,Mathew Suffoletto,Randall C. Starling,Cynthia Oblak,Leslie T. Cooper,Annette McNallan,Lisa R. Koenig,Paul Mather,Natalie Pierson,Sharon Rubin,Yanique Bell,Alicia Ervin,John Boehmer,Patricia Frey,Jeffrey D. Alexis,Janice Schrack,Pam LaDuke,Guillermo Torre‐Amione,Jeannie Arredondo,Daniel F. Pauly,Pamela Smith,Richard Sheppard,Stephanie Fuoco,Ilan S. Wittstein,Elayne Breton,Vinay Thohan,Deborah J. Wesley,G. William Dec,Diane Cocca-Spofford,David W. Markham,Lynn Fernandez,Colleen Debes,Mark Zucker,Laura L. Adams,Peter Liu,Judith Renton,Jagat Narula,Byron J. Allen,Elizabeth Westberg
出处
期刊:Jacc-Heart Failure [Elsevier]
卷期号:11 (9): 1231-1242 被引量:3
标识
DOI:10.1016/j.jchf.2023.05.031
摘要

The pathophysiology of peripartum cardiomyopathy (PPCM) and its distinctive biological features remain incompletely understood. High-throughput serum proteomic profiling, a powerful tool to gain insights into the pathophysiology of diseases at a systems biology level, has never been used to investigate PPCM relative to nonischemic cardiomyopathy.The aim of this study was to characterize the pathophysiology of PPCM through serum proteomic analysis.Aptamer-based proteomic analysis (SomaScan 7K) was performed on serum samples from women with PPCM (n = 67), women with nonischemic nonperipartum cardiomyopathy (NPCM) (n = 31), and age-matched healthy peripartum and nonperipartum women (n = 10 each). Serum samples were obtained from the IPAC (Investigation of Pregnancy-Associated Cardiomyopathy) and IMAC2 (Intervention in Myocarditis and Acute Cardiomyopathy) studies.Principal component analysis revealed unique clustering of each patient group (P for difference <0.001). Biological pathway analyses of differentially measured proteins in PPCM relative to NPCM, before and after normalization to pertinent healthy controls, highlighted specific dysregulation of inflammatory pathways in PPCM, including the upregulation of the cholesterol metabolism-related anti-inflammatory pathway liver-X receptor/retinoid-X receptor (LXR/RXR) (P < 0.01, Z-score 1.9-2.1). Cardiac recovery by 12 months in PPCM was associated with the downregulation of pro-inflammatory pathways and the upregulation of LXR/RXR, and an additional RXR-dependent pathway involved in the regulation of inflammation and metabolism, peroxisome proliferator-activated receptor α/RXRα signaling.Serum proteomic profiling of PPCM relative to NPCM and healthy controls indicated that PPCM is a distinct disease entity characterized by the unique dysregulation of inflammation-related pathways and cholesterol metabolism-related anti-inflammatory pathways. These findings provide insight into the pathophysiology of PPCM and point to novel potential therapeutic targets.
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