Complement Factor D Targeting Protects Endotheliopathy in Organoid and Monkey Models of COVID-19

Overview

Journal Cell Stem Cell

Publisher Cell Press

Specialty Cell Biology

Date 2023 Oct 6

PMID 37802037

Authors

Eri Kawakami

Norikazu Saiki

Yosuke Yoneyama

Chiharu Moriya

Mari Maezawa

Shuntaro Kawamura

Akiko Kinebuchi

Tamaki Kono

Masaaki Funata

Ayaka Sakoda

Shigeru Kondo

Takeshi Ebihara

Hisatake Matsumoto

Yuki Togami

Hiroshi Ogura

Fuminori Sugihara

Daisuke Okuzaki

Takashi Kojima

Sayaka Deguchi

Sebastien Vallee

Susan McQuade

Rizwana Islam

Madhusudan Natarajan

Hirohito Ishigaki

Misako Nakayama

Cong Thanh Nguyen

Yoshinori Kitagawa

Yunheng Wu

Kensaku Mori

Takayuki Hishiki

Tomohiko Takasaki

Yasushi Itoh

Kazuo Takayama

Yasunori Nio

Takanori Takebe

Affiliations

Soon will be listed here.

Abstract

COVID-19 is linked to endotheliopathy and coagulopathy, which can result in multi-organ failure. The mechanisms causing endothelial damage due to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) remain elusive. Here, we developed an infection-competent human vascular organoid from pluripotent stem cells for modeling endotheliopathy. Longitudinal serum proteome analysis identified aberrant complement signature in critically ill patients driven by the amplification cycle regulated by complement factor B and D (CFD). This deviant complement pattern initiates endothelial damage, neutrophil activation, and thrombosis specific to organoid-derived human blood vessels, as verified through intravital imaging. We examined a new long-acting, pH-sensitive (acid-switched) antibody targeting CFD. In both human and macaque COVID-19 models, this long-acting anti-CFD monoclonal antibody mitigated abnormal complement activation, protected endothelial cells, and curtailed the innate immune response post-viral exposure. Collectively, our findings suggest that the complement alternative pathway exacerbates endothelial injury and inflammation. This underscores the potential of CFD-targeted therapeutics against severe viral-induced inflammathrombotic outcomes.

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