Sequential Defects in Cardiac Lineage Commitment and Maturation Cause Hypoplastic Left Heart Syndrome

Markus Krane; Martina Dreßen; Gianluca Santamaria; Ilaria My; Christine M Schneider; Tatjana Dorn; Svenja Laue; Elisa Mastantuono; Riccardo Berutti; Hilansi Rawat; Ralf Gilsbach; Pedro Schneider; Harald Lahm; Sascha Schwarz; Stefanie A Doppler; Sharon Paige; Nazan Puluca; Sophia Doll; Irina Neb; Thomas Brade; Zhong Zhang; Claudia Abou-Ajram; Bernd Northoff; Lesca M Holdt; Stefanie Sudhop; Makoto Sahara; Alexander Goedel; Andreas Dendorfer; Fleur V Y Tjong; Maria E Rijlaarsdam; Julie Cleuziou; Nora Lang; Christian Kupatt; Connie Bezzina; Rüdiger Lange; Neil E Bowles; Matthias Mann; Bruce D Gelb; Lia Crotti; Lutz Hein; Thomas Meitinger; Sean Wu; Daniel Sinnecker; Peter J Gruber; Karl-Ludwig Laugwitz; Alessandra Moretti

doi:10.1161/CIRCULATIONAHA.121.056198

Sequential Defects in Cardiac Lineage Commitment and Maturation Cause Hypoplastic Left Heart Syndrome

Circulation. 2021 Oct 26;144(17):1409-1428. doi: 10.1161/CIRCULATIONAHA.121.056198. Epub 2021 Oct 25.

Authors

Markus Krane^#^{1

2}, Martina Dreßen^#¹, Gianluca Santamaria^#³, Ilaria My^#³, Christine M Schneider^#³, Tatjana Dorn^#³, Svenja Laue^#³, Elisa Mastantuono^{4

3

5}, Riccardo Berutti^{4

5}, Hilansi Rawat³, Ralf Gilsbach^{6

7

8}, Pedro Schneider⁶, Harald Lahm¹, Sascha Schwarz⁹, Stefanie A Doppler¹, Sharon Paige¹⁰, Nazan Puluca¹, Sophia Doll¹¹, Irina Neb¹, Thomas Brade³, Zhong Zhang¹, Claudia Abou-Ajram¹, Bernd Northoff¹², Lesca M Holdt¹², Stefanie Sudhop⁹, Makoto Sahara¹³, Alexander Goedel³, Andreas Dendorfer^{2

14}, Fleur V Y Tjong¹⁵, Maria E Rijlaarsdam¹⁶, Julie Cleuziou¹⁷, Nora Lang¹⁸, Christian Kupatt^{3

2}, Connie Bezzina¹⁵, Rüdiger Lange^{1

2}, Neil E Bowles¹⁹, Matthias Mann¹¹, Bruce D Gelb²⁰, Lia Crotti^{21

22

23}, Lutz Hein^{6

24}, Thomas Meitinger^{4

2

5}, Sean Wu¹⁰, Daniel Sinnecker^{3

2}, Peter J Gruber²⁵, Karl-Ludwig Laugwitz^{3

2}, Alessandra Moretti^{3

2}

Affiliations

¹ Department of Cardiovascular Surgery, Institute Insure (M.K., M.D., H.L., S.A.D., N.P., I.N., Z.Z., C.A.-A., R.L.),Klinikum rechts der Isar, School of Medicine & Health, Technical University of Munich, Germany.
² DZHK (German Centre for Cardiovascular Research)-partner site Munich Heart Alliance, Germany (M.K., A.D., C.K., R.L., T.M., D.S., K.-L.L., A.M.).
³ Department of Internal Medicine I, Cardiology (G.S., I.M., C.M.S., T.D., S.L., E.M., H.R., T.B., A.G., C.K., D.S., K.-L.L., A.M.), Klinikum rechts der Isar, School of Medicine & Health, Technical University of Munich, Germany.
⁴ German Heart Center Munich, and Institute of Human Genetics (E.M., R.B., T.M.), Klinikum rechts der Isar, School of Medicine & Health, Technical University of Munich, Germany.
⁵ Helmholtz Zentrum München, Neuherberg, Germany (E.M., R.B., T.M.).
⁶ Institute of Experimental and Clinical Pharmacology and Toxicology (R.G., P.S., L.H.), University of Freiburg, Germany.
⁷ Institute for Cardiovascular Physiology, Goethe University, Frankfurt am Main, Germany (R.G.).
⁸ DZHK (German Centre for Cardiovascular Research)-partner site RheinMain, Frankfurt am Main, Germany (R.G.).
⁹ Center for Applied Tissue Engineering and Regenerative Medicine (CANTER), Munich University of Applied Sciences, Germany (S. Schwarz, S. Sudhop).
¹⁰ Cardiovascular Institute, Stanford University School of Medicine, CA (S.P., S.W.).
¹¹ Proteomics and Signal Transduction, Max-Planck Institute of Biochemistry, Martinsried, Germany (S.D., M.M.).
¹² Institute of Laboratory Medicine (B.N., L.M.H.), University Hospital, LMU Munich, Germany.
¹³ Department of Cell and Molecular Biology, Karolinska Institute, Stockholm, Sweden (M.S.).
¹⁴ Walter-Brendel-Centre of Experimental Medicine (A.D.), University Hospital, LMU Munich, Germany.
¹⁵ Heart Centre, Department of Clinical and Experimental Cardiology, Amsterdam UMC, University of Amsterdam, The Netherlands (F.V.Y.T., C.B.).
¹⁶ Department of Pediatric Cardiology, Leiden University Medical Center, The Netherlands (M.E.R.).
¹⁷ Department of Congenital and Paediatric Heart Surgery, Institute Insure (J.C.), Klinikum rechts der Isar, School of Medicine & Health, Technical University of Munich, Germany.
¹⁸ Department of Paediatric Cardiology and Congenital Heart Defects (N.L.), Klinikum rechts der Isar, School of Medicine & Health, Technical University of Munich, Germany.
¹⁹ Department of Pediatrics (Division of Cardiology), University of Utah School of Medicine, Salt Lake City (N.E.B.).
²⁰ The Mindich Child Health and Development Institute, Icahn School of Medicine at Mount Sinai, New York (B.D.G.).
²¹ Center for Cardiac Arrhythmias of Genetic Origin and Laboratory of Cardiovascular Genetics, Istituto Auxologico Italiano, IRCCS, Milan, Italy (L.C.).
²² Cardiomyopathies Unit, Department of Cardiovascular, Neural and Metabolic Sciences, Istituto Auxologico Italiano, IRCCS, San Luca Hospital, Milan, Italy (L.C.).
²³ Department of Medicine and Surgery, University of Milano-Bicocca, Milan, Italy (L.C.).
²⁴ BIOSS, Center for Biological Signaling Studies (L.H.), University of Freiburg, Germany.
²⁵ Department of Surgery, Yale University, New Haven, CT (P.J.G.).

^# Contributed equally.

Abstract

Background: Complex molecular programs in specific cell lineages govern human heart development. Hypoplastic left heart syndrome (HLHS) is the most common and severe manifestation within the spectrum of left ventricular outflow tract obstruction defects occurring in association with ventricular hypoplasia. The pathogenesis of HLHS is unknown, but hemodynamic disturbances are assumed to play a prominent role.

Methods: To identify perturbations in gene programs controlling ventricular muscle lineage development in HLHS, we performed whole-exome sequencing of 87 HLHS parent-offspring trios, nuclear transcriptomics of cardiomyocytes from ventricles of 4 patients with HLHS and 15 controls at different stages of heart development, single cell RNA sequencing, and 3D modeling in induced pluripotent stem cells from 3 patients with HLHS and 3 controls.

Results: Gene set enrichment and protein network analyses of damaging de novo mutations and dysregulated genes from ventricles of patients with HLHS suggested alterations in specific gene programs and cellular processes critical during fetal ventricular cardiogenesis, including cell cycle and cardiomyocyte maturation. Single-cell and 3D modeling with induced pluripotent stem cells demonstrated intrinsic defects in the cell cycle/unfolded protein response/autophagy hub resulting in disrupted differentiation of early cardiac progenitor lineages leading to defective cardiomyocyte subtype differentiation/maturation in HLHS. Premature cell cycle exit of ventricular cardiomyocytes from patients with HLHS prevented normal tissue responses to developmental signals for growth, leading to multinucleation/polyploidy, accumulation of DNA damage, and exacerbated apoptosis, all potential drivers of left ventricular hypoplasia in absence of hemodynamic cues.

Conclusions: Our results highlight that despite genetic heterogeneity in HLHS, many mutations converge on sequential cellular processes primarily driving cardiac myogenesis, suggesting novel therapeutic approaches.

Keywords: autophagy; cell cycle; heart defects, congenital; hypoplastic left heart syndrome; induced pluripotent stem cells; unfolded protein response; whole exome sequencing.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Genetic Heterogeneity
Humans
Hypoplastic Left Heart Syndrome / genetics*
Organogenesis / genetics*

Grants and funding

UL1 TR001863/TR/NCATS NIH HHS/United States