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A new murine model of Barth Syndrome neutropenia links TAFAZZIN deficiency to increased ER stress induced apoptosis

Authors :
Jihee Sohn
Jelena Milosevic
Thomas Brouse
Najihah Aziz
Jenna Elkhoury
Suya Wang
Alexander Hauschild
Nick van Gastel
Murat Cetinbas
Sara F. Tufa
Douglas R. Keene
Ruslan I. Sadreyev
William T. Pu
David B. Sykes
Massachusetts General Hospital - Center for Regenerative Medicine
Boston Children’s Hospital - Department of Cardiology
UCL - SSS/DDUV - Institut de Duve
Harvard University - Harvard Stem Cell Institute
Massachusetts General Hospital - Department of Molecular Biology
Harvard Medical School - Department of Genetics
Shriners Hospitals for Children - Micro-Imaging Center
Massachusetts General Hospital - Department of Pathology
Massachusetts General Hospital - Cancer Center
Source :
Blood advances, (2022)
Publication Year :
2022

Abstract

Barth syndrome is an inherited X-linked disorder that leads to cardiomyopathy, skeletal myopathy, and neutropenia. These symptoms result from the loss of function of the enzyme TAFAZZIN, a transacylase located in the inner mitochondrial membrane that is responsible for the final steps of cardiolipin production. The link between defective cardiolipin maturation and neutropenia remains unclear. To address potential mechanisms of neutropenia, we examined myeloid progenitor development within the fetal liver of TAFAZZIN knockout (KO) animals as well as within the adult bone marrow of wild-type recipients transplanted with TAFAZZIN-KO hematopoietic stem cells. We also used the ER-Hoxb8 system (estrogen receptor fused to Hoxb8) of conditional immortalization to establish a new murine model system for the ex vivo study of TAFAZZIN-deficient neutrophils. The TAFAZZIN-KO cells demonstrated the expected dramatic differences in cardiolipin maturation that result from a lack of TAFAZZIN enzyme activity. Contrary to our hypothesis, we did not identify any significant differences in neutrophil development or neutrophil function across a variety of assays including phagocytosis and the production of cytokines or reactive oxygen species. However, transcriptomic analysis of the TAFAZZIN-deficient neutrophil progenitors demonstrated an upregulation of markers of endoplasmic reticulum stress and confirmatory testing demonstrated that the TAFAZZIN-deficient cells had increased sensitivity to certain ER stress-mediated and non-ER stress-mediated triggers of apoptosis. Although the link between increased sensitivity to apoptosis and the variably penetrant neutropenia phenotype seen in some patients with Barth syndrome remains to be clarified, our studies and new model system set a foundation for further investigation.

Details

Language :
English
Database :
OpenAIRE
Journal :
Blood advances, (2022)
Accession number :
edsair.doi.dedup.....f49de05b647a9f645324a100d38d6ae3