作者
Priti Azad, Andrew B Caldwell, Srinivasan Ramachandran, Nathanael J Spann, Ali Akbari, Francisco C Villafuerte, Daniela Bermudez, Helen Zhao, Orit Poulsen, Dan Zhou, Vineet Bafna, Shankar Subramaniam, Gabriel G Haddad
发表日期
2022/6
期刊
Experimental & molecular medicine
卷号
54
期号
6
页码范围
777-787
出版商
Nature Publishing Group UK
简介
At high altitude Andean region, hypoxia-induced excessive erythrocytosis (EE) is the defining feature of Monge’s disease or chronic mountain sickness (CMS). At the same altitude, resides a population that has developed adaptive mechanism(s) to constrain this hypoxic response (non-CMS). In this study, we utilized an in vitro induced pluripotent stem cell model system to study both populations using genomic and molecular approaches. Our whole genome analysis of the two groups identified differential SNPs between the CMS and non-CMS subjects in the ARID1B region. Under hypoxia, the expression levels of ARID1B significantly increased in the non-CMS cells but decreased in the CMS cells. At the molecular level, ARID1B knockdown (KD) in non-CMS cells increased the levels of the transcriptional regulator GATA1 by 3-fold and RBC levels by 100-fold under hypoxia. ARID1B KD in non-CMS cells led to …
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