Shuang Zhang1, Xin-Yi Yeap1, Lubov Grigoryeva1, Shirley Dehn1, Matthew DeBerge1, Michael Tye1, Emily Rostlund1, Dorien Schrijvers2, Zheng Jenny Zhang2, Ronen Sumagin3, Warren G Tourtellotte1, Daniel Lee3, Jon Lomasney1, John Morrow4, Edward B Thorp5. 1. Feinberg Cardiovascular Research Institute, Northwestern University, Chicago, IL, USA; Surgery-Organ Transplantation, Northwestern University, Chicago, IL, USA. 2. University of Antwerp, Belgium. 3. Feinberg Cardiovascular Research Institute, Northwestern University, Chicago, IL, USA. 4. Department of Cardiology and Division of Molecular Medicine, Columbia University, New York, NY, USA. 5. Feinberg Cardiovascular Research Institute, Northwestern University, Chicago, IL, USA; Surgery-Organ Transplantation, Northwestern University, Chicago, IL, USA. Electronic address: ebthorp@northwestern.edu.
Abstract
BACKGROUND: Mobilization of the innate immune response to clear and metabolize necrotic and apoptotic cardiomyocytes is a prerequisite to heart repair after cardiac injury. Suboptimal kinetics of dying myocyte clearance leads to secondary necrosis, and in the case of the heart, increased potential for collateral loss of neighboring non-regenerative myocytes. Despite the importance of myocyte phagocytic clearance during heart repair, surprisingly little is known about its underlying cell and molecular biology. OBJECTIVE: To determine if phagocytic receptor MERTK is expressed in human hearts and to elucidate key sequential steps and phagocytosis efficiency of dying adult cardiomyocytes, by macrophages. RESULTS: In infarcted human hearts, expression profiles of the phagocytic receptor MER-tyrosine kinase (MERTK) mimicked that found in experimental ischemic mouse hearts. Electron micrographs of myocardium identified MERTK signal along macrophage phagocytic cups and Mertk-/- macrophages contained reduced digested myocyte debris after myocardial infarction. Ex vivo co-culture of primary macrophages and adult cardiomyocyte apoptotic bodies revealed reduced engulfment relative to resident cardiac fibroblasts. Inefficient clearance was not due to the larger size of myocyte apoptotic bodies, nor were other key steps preceding the formation of phagocytic synapses significantly affected; this included macrophage chemotaxis and direct binding of phagocytes to myocytes. Instead, suppressed phagocytosis was directly associated with myocyte-induced inactivation of MERTK, which was partially rescued by genetic deletion of a MERTK proteolytic susceptibility site. CONCLUSION: Utilizing an ex vivo co-cultivation approach to model key cellular and molecular events found in vivo during infarction, cardiomyocyte phagocytosis was found to be inefficient, in part due to myocyte-induced shedding of macrophage MERTK. These findings warrant future studies to identify other cofactors of macrophage-cardiomyocyte cross-talk that contribute to cardiac pathophysiology.
BACKGROUND: Mobilization of the innate immune response to clear and metabolize necrotic and apoptotic cardiomyocytes is a prerequisite to heart repair after cardiac injury. Suboptimal kinetics of dying myocyte clearance leads to secondary necrosis, and in the case of the heart, increased potential for collateral loss of neighboring non-regenerative myocytes. Despite the importance of myocyte phagocytic clearance during heart repair, surprisingly little is known about its underlying cell and molecular biology. OBJECTIVE: To determine if phagocytic receptor MERTK is expressed in human hearts and to elucidate key sequential steps and phagocytosis efficiency of dying adult cardiomyocytes, by macrophages. RESULTS: In infarctedhuman hearts, expression profiles of the phagocytic receptor MER-tyrosine kinase (MERTK) mimicked that found in experimental ischemicmouse hearts. Electron micrographs of myocardium identified MERTK signal along macrophage phagocytic cups and Mertk-/- macrophages contained reduced digested myocyte debris after myocardial infarction. Ex vivo co-culture of primary macrophages and adult cardiomyocyte apoptotic bodies revealed reduced engulfment relative to resident cardiac fibroblasts. Inefficient clearance was not due to the larger size of myocyte apoptotic bodies, nor were other key steps preceding the formation of phagocytic synapses significantly affected; this included macrophage chemotaxis and direct binding of phagocytes to myocytes. Instead, suppressed phagocytosis was directly associated with myocyte-induced inactivation of MERTK, which was partially rescued by genetic deletion of a MERTK proteolytic susceptibility site. CONCLUSION: Utilizing an ex vivo co-cultivation approach to model key cellular and molecular events found in vivo during infarction, cardiomyocyte phagocytosis was found to be inefficient, in part due to myocyte-induced shedding of macrophage MERTK. These findings warrant future studies to identify other cofactors of macrophage-cardiomyocyte cross-talk that contribute to cardiac pathophysiology.
Authors: Elaine Wan; Xin Yi Yeap; Shirley Dehn; Rachael Terry; Margaret Novak; Shuang Zhang; Shinichi Iwata; Xiaoqiang Han; Shunichi Homma; Konstantinos Drosatos; Jon Lomasney; David M Engman; Stephen D Miller; Douglas E Vaughan; John P Morrow; Raj Kishore; Edward B Thorp Journal: Circ Res Date: 2013-07-08 Impact factor: 17.367
Authors: Slava Epelman; Kory J Lavine; Anna E Beaudin; Dorothy K Sojka; Javier A Carrero; Boris Calderon; Thaddeus Brija; Emmanuel L Gautier; Stoyan Ivanov; Ansuman T Satpathy; Joel D Schilling; Reto Schwendener; Ismail Sergin; Babak Razani; E Camilla Forsberg; Wayne M Yokoyama; Emil R Unanue; Marco Colonna; Gwendalyn J Randolph; Douglas L Mann Journal: Immunity Date: 2014-01-16 Impact factor: 31.745
Authors: Shuang Zhang; Samuel Weinberg; Matthew DeBerge; Anastasiia Gainullina; Matthew Schipma; Jason M Kinchen; Issam Ben-Sahra; David R Gius; Laurent Yvan-Charvet; Navdeep S Chandel; Paul T Schumacker; Edward B Thorp Journal: Cell Metab Date: 2018-12-27 Impact factor: 27.287
Authors: Shuang Zhang; Xin-Yi Yeap; Matthew DeBerge; Nivedita K Naresh; Kevin Wang; Zhengxin Jiang; Jane E Wilcox; Steven M White; John P Morrow; Paul W Burridge; Daniel Procissi; Evan A Scott; William Frazier; Edward B Thorp Journal: JACC Basic Transl Sci Date: 2017-08
Authors: Matthew DeBerge; Shuang Zhang; Kristofor Glinton; Luba Grigoryeva; Islam Hussein; Esther Vorovich; Karen Ho; Xunrong Luo; Edward B Thorp Journal: Front Immunol Date: 2017-11-01 Impact factor: 7.561
Authors: Xuezhou Hou; Guobao Chen; William Bracamonte-Baran; Hee Sun Choi; Nicola L Diny; Jungeun Sung; David Hughes; Taejoon Won; Megan Kay Wood; Monica V Talor; David Joel Hackam; Karin Klingel; Giovanni Davogustto; Heinrich Taegtmeyer; Isabelle Coppens; Jobert G Barin; Daniela Čiháková Journal: Cell Rep Date: 2019-07-02 Impact factor: 9.423