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Lymphoangiocrine signals promote cardiac growth and repair.

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dc.contributor.authorLiu, Xiaolei
dc.contributor.authorDe la Cruz, Ester
dc.contributor.authorGu, Xiaowu
dc.contributor.authorBalint, Laszlo
dc.contributor.authorOxendine-Burns, Michael
dc.contributor.authorTerrones, Tamara
dc.contributor.authorMa, Wanshu
dc.contributor.authorKuo, Hui-Hsuan
dc.contributor.authorLantz, Connor
dc.contributor.authorBansal, Trisha
dc.contributor.authorThorp, Edward
dc.contributor.authorBurridge, Paul
dc.contributor.authorJakus, Zoltán
dc.contributor.authorHerz, Joachim
dc.contributor.authorCleaver, Ondine
dc.contributor.authorTorres, Miguel
dc.contributor.authorOliver, Guillermo
dc.contributor.funderMinisterio de Educación (España)es_ES
dc.contributor.funderEuropean Molecular Biology Organizationes_ES
dc.contributor.funderMinisterio de Ciencia e Innovación (España)es_ES
dc.contributor.funderNational Institutes of Health (Estados Unidos)es_ES
dc.date.accessioned2022-12-01T15:17:52Z
dc.date.available2022-12-01T15:17:52Z
dc.date.issued2020-12
dc.descriptionThis work was supported by NIH grant (RO1HL073402-16) to G.O, AHA grant (18CDA34110356) to X.L, 5T32HL134633 to W.M, FPU grant from the Spanish Ministry of Education, Culture and Sports and EMBO ShortTerm Fellowship to E.C.C, Leducq TNE-17CVD and RD16/0011/0019 (ISCIII) from the Spanish Ministry of Science, Innovation, and Universities to M.T, NIH T32 GM008061 to C.L, HL63762, and NS093382 to J.H. We thank Dr. Gabriele M. Rune and Dr. Bianka Brunne for the Reln +/− strain. RNAseq work was supported by the Northwestern University NUSeq Core Facility. We thank the Robert H. Lurie Cancer Center Flow Cytometry facility supported by NCI CCSG P30 CA060553 for their invaluable assistance. Flow Cytometry Cell Sorting was performed on a BD FACSAria SORP system and BD FACSymphony S6 SORP system, purchased through the support of NIH 1S10OD011996-01 and 1S10OD026814-01. Imaging work was performed at the Northwestern University Center for Advanced Microscopy supported by NCI CCSG P30 CA060553 awarded to the Robert H Lurie Comprehensive Cancer Center. Spinning disk confocal microscopy was performed on an Andor XDI Revolution microscope, purchased through the support of NCRR 1S10 RR031680-01. Proteomics services were performed by the Northwestern Proteomics Core Facility supported by NCI CCSG P30 CA060553 awarded to the Robert H Lurie Comprehensive Cancer Center, instrumentation award (S10OD025194) from NIH Office of Director, and the National Resource for Translational and Developmental Proteomics supported by P41 GM108569. We thank the George M. O’Brien Kidney Research Core Center (NU GoKidney, supported by a P30 DK114857 award from NIDDK) for the use of the Echocardiography machine. The myocardial infarction surgeries were performed by the comprehensive Transplant Center Microsurgery Core, partially supported by NIH NIAID P01AI112522. We thank Dr. Jing Jin and Dr. Pan Liu for help with the ELISA reagents and data analysis, Dr. Ruihua Ma for help with DNA polyploidy analysis, Ao Shi for the Mef2c antibodies, Dr. Michael Dellinger for the Prox1CreERT2 mice and Dr. Hossein Ardehali for the MhcCre mice. We specially thank Dr. Beatriz Sosa-Pineda for advice and valuable suggestions and Dr. Pilar Ruiz-Lozano for shearing her expertise in the preparation of the collagen patches.es_ES
dc.description.abstractRecent studies have suggested that lymphatics help to restore heart function after cardiac injury1-6. Here we report that lymphatics promote cardiac growth, repair and cardioprotection in mice. We show that a lymphoangiocrine signal produced by lymphatic endothelial cells (LECs) controls the proliferation and survival of cardiomyocytes during heart development, improves neonatal cardiac regeneration and is cardioprotective after myocardial infarction. Embryos that lack LECs develop smaller hearts as a consequence of reduced cardiomyocyte proliferation and increased cardiomyocyte apoptosis. Culturing primary mouse cardiomyocytes in LEC-conditioned medium increases cardiomyocyte proliferation and survival, which indicates that LECs produce lymphoangiocrine signals that control cardiomyocyte homeostasis. Characterization of the LEC secretome identified the extracellular protein reelin (RELN) as a key component of this process. Moreover, we report that LEC-specific Reln-null mouse embryos develop smaller hearts, that RELN is required for efficient heart repair and function after neonatal myocardial infarction, and that cardiac delivery of RELN using collagen patches improves heart function in adult mice after myocardial infarction by a cardioprotective effect. These results highlight a lymphoangiocrine role of LECs during cardiac development and injury response, and identify RELN as an important mediator of this function.es_ES
dc.description.peerreviewedes_ES
dc.format.number7839es_ES
dc.format.page705es_ES
dc.format.volume588es_ES
dc.identifier.citationNature . 2020 Dec;588(7839):705-711.es_ES
dc.identifier.doi10.1038/s41586-020-2998-xes_ES
dc.identifier.e-issn1476-4687es_ES
dc.identifier.journalNaturees_ES
dc.identifier.pubmedID33299187es_ES
dc.identifier.urihttp://hdl.handle.net/20.500.12105/15252
dc.language.isoenges_ES
dc.publisherNature Publishing Groupes_ES
dc.relation.projectFECYTinfo:eu-repo/grantAgreement/MINECO//RD16%2F0011%2F0019/ES/Red de Terapia Celular (TerCel)/
dc.relation.publisherversion10.1038/s41586-020-2998-xes_ES
dc.repisalud.institucionCNICes_ES
dc.repisalud.orgCNICCNIC::Grupos de investigación::Control Genético del Desarrollo y Regeneración de Órganoses_ES
dc.rights.accessRightsopen accesses_ES
dc.rights.licenseAtribución 4.0 Internacional*
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/*
dc.subject.meshRegenerationes_ES
dc.subject.meshSignal Transductiones_ES
dc.subject.meshAnimalses_ES
dc.subject.meshAnimals, Newbornes_ES
dc.subject.meshApoptosises_ES
dc.subject.meshCell Adhesion Molecules, Neuronales_ES
dc.subject.meshCell Proliferationes_ES
dc.subject.meshCell Survivales_ES
dc.subject.meshCells, Culturedes_ES
dc.subject.meshEndothelial Cellses_ES
dc.subject.meshExtracellular Matrix Proteinses_ES
dc.subject.meshFemalees_ES
dc.subject.meshHeartes_ES
dc.subject.meshHumanses_ES
dc.subject.meshIntegrin beta1es_ES
dc.subject.meshLymphatic Systemes_ES
dc.subject.meshMicees_ES
dc.subject.meshMyocardial Infarctiones_ES
dc.subject.meshMyocardiumes_ES
dc.subject.meshMyocytes, Cardiaces_ES
dc.subject.meshNerve Tissue Proteinses_ES
dc.subject.meshOrgan Sizees_ES
dc.subject.meshOrganogenesises_ES
dc.subject.meshReelin Proteines_ES
dc.subject.meshSerine Endopeptidaseses_ES
dc.titleLymphoangiocrine signals promote cardiac growth and repair.es_ES
dc.typejournal articlees_ES
dc.type.hasVersionVoRes_ES
dspace.entity.typePublication
relation.isAuthorOfPublication6ec1130e-9194-41d3-b53f-eba5fc1af5c9
relation.isAuthorOfPublication.latestForDiscovery6ec1130e-9194-41d3-b53f-eba5fc1af5c9

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