SOX17 Deficiency Mediates Pulmonary Hypertension: At the Crossroads of Sex, Metabolism, and Genetics

Shreya Sangam; Xutong Sun; Tae-Hwi Schwantes-An; Manivannan Yegambaram; Qing Lu; Yinan Shi; Todd Cook; Amanda Fisher; Andrea L Frump; Anna Coleman; Yanan Sun; Shuxin Liang; Howard Crawford; Katie A Lutz; Avinash D Maun; Michael W Pauciulo; Jason H Karnes; Ketul R Chaudhary; Duncan J Stewart; Paul R Langlais; Mohit Jain; Mona Alotaibi; Tim Lahm; Yan Jin; Haiwei Gu; Haiyang Tang; William C Nichols; Stephen M Black; Ankit A Desai

doi:10.1164/rccm.202203-0450OC

SOX17 Deficiency Mediates Pulmonary Hypertension: At the Crossroads of Sex, Metabolism, and Genetics

Am J Respir Crit Care Med. 2023 Apr 15;207(8):1055-1069. doi: 10.1164/rccm.202203-0450OC.

Authors

Shreya Sangam^{1

2}, Xutong Sun^{3

4}, Tae-Hwi Schwantes-An⁵, Manivannan Yegambaram^{3

4}, Qing Lu^{3

4}, Yinan Shi^{1

6}, Todd Cook¹, Amanda Fisher¹, Andrea L Frump¹, Anna Coleman^{7

8}, Yanan Sun^{6

9}, Shuxin Liang⁶, Howard Crawford¹⁰, Katie A Lutz^{7

8}, Avinash D Maun¹, Michael W Pauciulo^{7

8}, Jason H Karnes¹¹, Ketul R Chaudhary¹², Duncan J Stewart¹³, Paul R Langlais¹⁴, Mohit Jain¹, Mona Alotaibi^{1

15}, Tim Lahm^{1

16

17}, Yan Jin^{3

4}, Haiwei Gu^{3

4}, Haiyang Tang⁶, William C Nichols^{7

8}, Stephen M Black^{3

4

18}, Ankit A Desai¹

Affiliations

¹ Department of Medicine and.
² Department of Clinical Translational Sciences.
³ Center for Translational Science, Florida International University, Port Saint Lucie, Florida.
⁴ Department of Environmental Health Sciences, Robert Stempel College of Public Health and Social Work, and.
⁵ Department of Medical & Molecular Genetics, Indiana University, Indianapolis, Indiana.
⁶ State Key Laboratory of Respiratory Disease, National Clinical Research Center for Respiratory Disease, Guangdong Key Laboratory of Vascular Disease, Guangzhou Institute of Respiratory Health, The First Affiliated Hospital of Guangzhou Medical University, Guangzhou, China.
⁷ Division of Human Genetics, Cincinnati Children's Hospital Medical Center and.
⁸ Department of Pediatrics, University of Cincinnati College of Medicine, Cincinnati, Ohio.
⁹ College of Veterinary Medicine, Northwest A & F University, Yangling, China.
¹⁰ Henry Ford Pancreatic Cancer Center, Henry Ford Hospital, Detroit, Michigan.
¹¹ Department of Pharmacy Practice and Science, R. Ken Coit College of Pharmacy, and.
¹² Department of Physiology and Biophysics, Dalhousie University, Halifax, Nova Scotia, Canada.
¹³ Department of Medicine, Ottawa Hospital Research Institute, Ottawa, Ontario, Canada.
¹⁴ Division of Endocrinology, College of Medicine, University of Arizona, Tucson, Arizona.
¹⁵ Division of Pulmonary, Critical Care and Sleep Medicine, University of California, San Diego, La Jolla, California.
¹⁶ Richard L. Roudebush Veterans Affairs Medical Center, Indianapolis, Indiana; and.
¹⁷ Department of Medicine, National Jewish Health, Denver, Colorado.
¹⁸ Herbert Wertheim College of Medicine, Florida International University, Miami, Florida.

Abstract

Rationale: Genetic studies suggest that SOX17 (SRY-related HMG-box 17) deficiency increases pulmonary arterial hypertension (PAH) risk. Objectives: On the basis of pathological roles of estrogen and HIF2α (hypoxia-inducible factor 2α) signaling in pulmonary artery endothelial cells (PAECs), we hypothesized that SOX17 is a target of estrogen signaling that promotes mitochondrial function and attenuates PAH development via HIF2α inhibition. Methods: We used metabolic (Seahorse) and promoter luciferase assays in PAECs together with the chronic hypoxia murine model to test the hypothesis. Measurements and Main Results: Sox17 expression was reduced in PAH tissues (rodent models and from patients). Chronic hypoxic pulmonary hypertension was exacerbated by mice with conditional Tie2-Sox17 (Sox17^EC-/-) deletion and attenuated by transgenic Tie2-Sox17 overexpression (Sox17^Tg). On the basis of untargeted proteomics, metabolism was the top pathway altered by SOX17 deficiency in PAECs. Mechanistically, we found that HIF2α concentrations were increased in the lungs of Sox17^EC-/- and reduced in those from Sox17^Tg mice. Increased SOX17 promoted oxidative phosphorylation and mitochondrial function in PAECs, which were partly attenuated by HIF2α overexpression. Rat lungs in males displayed higher Sox17 expression versus females, suggesting repression by estrogen signaling. Supporting 16α-hydroxyestrone (16αOHE; a pathologic estrogen metabolite)-mediated repression of SOX17 promoter activity, Sox17^Tg mice attenuated 16αOHE-mediated exacerbations of chronic hypoxic pulmonary hypertension. Finally, in adjusted analyses in patients with PAH, we report novel associations between a SOX17 risk variant, rs10103692, and reduced plasma citrate concentrations (n = 1,326). Conclusions: Cumulatively, SOX17 promotes mitochondrial bioenergetics and attenuates PAH, in part, via inhibition of HIF2α. 16αOHE mediates PAH development via downregulation of SOX17, linking sexual dimorphism and SOX17 genetics in PAH.

Keywords: 16α-hydroxyestrone; SRY-related HMG-box 17; hypoxia-inducible factor 2α; metabolism; pulmonary arterial hypertension.

Publication types

Research Support, U.S. Gov't, Non-P.H.S.
Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Endothelial Cells / metabolism
Estrogens
Familial Primary Pulmonary Hypertension / complications
Female
HMGB Proteins / metabolism
Hypertension, Pulmonary* / metabolism
Hypoxia / complications
Lung
Male
Mice
Pulmonary Arterial Hypertension* / metabolism
Pulmonary Artery
Rats
SOXF Transcription Factors / genetics

Substances

Estrogens
Sox17 protein, mouse
HMGB Proteins
SOXF Transcription Factors

Abstract

Publication types

MeSH terms

Substances

Grants and funding