Endothelial GNAQ p.R183Q Increases ANGPT2 (Angiopoietin-2) and Drives Formation of Enlarged Blood Vessels-Reference-Cited by-同舟云学术

Endothelial GNAQ p.R183Q Increases ANGPT2 (Angiopoietin-2) and Drives Formation of Enlarged Blood Vessels

Published:2022-01 Issue:1 Volume:42 Page:
ISSN:1079-5642
Container-title:Arteriosclerosis, Thrombosis, and Vascular Biology
language:en
Short-container-title:ATVB

Author:

Huang Lan¹²,Bichsel Colette¹²,Norris Alexis L.³,Thorpe Jeremy³,Pevsner Jonathan³,Alexandrescu Sanda⁴^ORCID,Pinto Anna⁵,Zurakowski David⁶,Kleiman Robin J.⁵,Sahin Mustafa⁵^ORCID,Greene Arin K.⁷⁸,Bischoff Joyce¹²^ORCID

Affiliation:

1. Vascular Biology Program (L.H., C.B., J.B.), Boston Children’s Hospital and Harvard Medical School, MA.

2. Department of Surgery (L.H., C.B., J.B.), Boston Children’s Hospital and Harvard Medical School, MA.

3. Department of Neurology, Kennedy Krieger Institute, Johns Hopkins University School of Medicine, Baltimore, MD (A.L.N., J.T., J.P.).

4. Department of Pathology (S.A.), Boston Children’s Hospital and Harvard Medical School, MA.

5. Department of Neurology (A.P., R.J.K., M.S.), Boston Children’s Hospital and Harvard Medical School, MA.

6. Department of Anesthesiology, Critical Care and Pain Medicine Research (D.Z.), Boston Children’s Hospital and Harvard Medical School, MA.

7. Department of Plastic and Oral Surgery (A.K.G.), Boston Children’s Hospital and Harvard Medical School, MA.

8. Vascular Anomalies Center (A.K.G.), Boston Children’s Hospital and Harvard Medical School, MA.

Abstract

Objective: Capillary malformation (CM) occurs sporadically and is associated with Sturge-Weber syndrome. The somatic mosaic mutation in GNAQ (c.548G>A, p.R183Q) is enriched in endothelial cells (ECs) in skin CM and Sturge-Weber syndrome brain CM. Our goal was to investigate how the mutant Gαq (G-protein αq subunit) alters EC signaling and disrupts capillary morphogenesis. Approach and Results: We used lentiviral constructs to express p.R183Q or wild-type GNAQ in normal human endothelial colony forming cells (EC-R183Q and EC-WT, respectively). EC-R183Q constitutively activated PLC (phospholipase C) β3, a downstream effector of Gαq. Activated PLCβ3 was also detected in human CM tissue sections. Bulk RNA sequencing analyses of mutant versus wild-type EC indicated constitutive activation of PKC (protein kinase C), NF-κB (nuclear factor kappa B) and calcineurin signaling in EC-R183Q. Increased expression of downstream targets in these pathways, ANGPT2 (angiopoietin-2) and DSCR (Down syndrome critical region protein) 1.4 were confirmed by quantitative PCR and immunostaining of human CM tissue sections. The Gαq inhibitor YM-254890 as well as siRNA targeted to PLCβ3 reduced mRNA expression levels of these targets in EC-R183Q while the pan-PKC inhibitor AEB071 reduced ANGPT2 but not DSCR1.4. EC-R183Q formed enlarged blood vessels in mice, reminiscent of those found in human CM. shRNA knockdown of ANGPT2 in EC-R183Q normalized the enlarged vessels to sizes comparable those formed by EC-WT. Conclusions: Gαq-R183Q, when expressed in ECs, establishes constitutively active PLCβ3 signaling that leads to increased ANGPT2 and a proangiogenic, proinflammatory phenotype. EC-R183Q are sufficient to form enlarged CM-like vessels in mice, and suppression of ANGPT2 prevents the enlargement. Our study provides the first evidence that endothelial Gαq-R183Q is causative for CM and identifies ANGPT2 as a contributor to CM vascular phenotype.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

Link

https://www.ahajournals.org/doi/pdf/10.1161/ATVBAHA.121.316651

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