Start Over

GLI1+ Cells Contribute to Vascular Remodeling in Pulmonary Hypertension.

Authors :: Chu X
Kheirollahi V
Lingampally A
Chelladurai P
Valasarajan C
Vazquez-Armendariz AI
Hadzic S
Khadim A
Pak O
Rivetti S
Wilhelm J
Bartkuhn M
Crnkovic S
Moiseenko A
Heiner M
Kraut S
Atefi LS
Koepke J
Valente G
Ruppert C
Braun T
Samakovlis C
Alexopoulos I
Looso M
Chao CM
Herold S
Seeger W
Kwapiszewska G
Huang X
Zhang JS
Pullamsetti SS
Weissmann N
Li X
El Agha E
Bellusci S
Source :: Circulation research [Circ Res] 2024 May 24; Vol. 134 (11), pp. e133-e149. Date of Electronic Publication: 2024 Apr 19.
Publication Year :: 2024
Abstract: Background: The precise origin of newly formed ACTA2+ (alpha smooth muscle actin-positive) cells appearing in nonmuscularized vessels in the context of pulmonary hypertension is still debatable although it is believed that they predominantly derive from preexisting vascular smooth muscle cells (VSMCs).<br />Methods: Gli1 <superscript> Cre-ERT2 </superscript> ; tdTomato <superscript> flox </superscript> mice were used to lineage trace GLI1+ (glioma-associated oncogene homolog 1-positive) cells in the context of pulmonary hypertension using 2 independent models of vascular remodeling and reverse remodeling: hypoxia and cigarette smoke exposure. Hemodynamic measurements, right ventricular hypertrophy assessment, flow cytometry, and histological analysis of thick lung sections followed by state-of-the-art 3-dimensional reconstruction and quantification using Imaris software were used to investigate the contribution of GLI1+ cells to neomuscularization of the pulmonary vasculature.<br />Results: The data show that GLI1+ cells are abundant around distal, nonmuscularized vessels during steady state, and this lineage contributes to around 50% of newly formed ACTA2+ cells around these normally nonmuscularized vessels. During reverse remodeling, cells derived from the GLI1+ lineage are largely cleared in parallel to the reversal of muscularization. Partial ablation of GLI1+ cells greatly prevented vascular remodeling in response to hypoxia and attenuated the increase in right ventricular systolic pressure and right heart hypertrophy. Single-cell RNA sequencing on sorted lineage-labeled GLI1+ cells revealed an Acta2 <superscript> high </superscript> fraction of cells with pathways in cancer and MAPK (mitogen-activated protein kinase) signaling as potential players in reprogramming these cells during vascular remodeling. Analysis of human lung-derived material suggests that GLI1 signaling is overactivated in both group 1 and group 3 pulmonary hypertension and can promote proliferation and myogenic differentiation.<br />Conclusions: Our data highlight GLI1+ cells as an alternative cellular source of VSMCs in pulmonary hypertension and suggest that these cells and the associated signaling pathways represent an important therapeutic target for further studies.<br />Competing Interests: Disclosures None.