Tissue Kallikrein in Cardiovascular, Cerebrovascular and Renal Diseases and Skin Wound Healing

Overview

Journal Biol Chem

Specialty Biochemistry

Date 2010 Feb 26

PMID 20180644

Citations 57

Authors

Julie Chao

Bo Shen

Lin Gao

Chun-Fang Xia

Grant Bledsoe

Lee Chao

Affiliations

Soon will be listed here.

Abstract

Tissue kallikrein (KLK1) processes low-molecular weight kininogen to produce vasoactive kinins, which exert biological functions via kinin receptor signaling. Using various delivery approaches, we have demonstrated that tissue kallikrein through kinin B2 receptor signaling exhibits a wide spectrum of beneficial effects by reducing cardiac and renal injuries, restenosis and ischemic stroke, and by promoting angiogenesis and skin wound healing, independent of blood pressure reduction. Protection by tissue kallikrein in oxidative organ damage is attributed to the inhibition of apoptosis, inflammation, hypertrophy and fibrosis. Tissue kallikrein also enhances neovascularization in ischemic heart and limb. Moreover, tissue kallikrein/kinin infusion not only prevents but also reverses kidney injury, inflammation and fibrosis in salt-induced hypertensive rats. Furthermore, there is a wide time window for kallikrein administration in protection against ischemic brain infarction, as delayed kallikrein infusion for 24 h after cerebral ischemia in rats is effective in reducing neurological deficits, infarct size, apoptosis and inflammation. Importantly, in the clinical setting, human tissue kallikrein has been proven to be effective in the treatment of patients with acute brain infarction when injected within 48 h after stroke onset. Finally, kallikrein promotes skin wound healing and keratinocyte migration by direct activation of protease-activated receptor 1.

Citing Articles

Tissue Kallikrein-1 Suppresses Type I Interferon Responses and Reduces Depressive-Like Behavior in the MRL/lpr Lupus-Prone Mouse Model.

Bhoj P, Nocito C, Togre N, Winfield M, Lubinsky C, Khan S Int J Mol Sci. 2024; 25(18).

PMID: 39337564 PMC: 11432477. DOI: 10.3390/ijms251810080.

The effectiveness and safety of human urinary kallidinogenase in acute ischemic stroke patients undergoing endovascular therapy.

Wang M, Guo C, Yang J, Li J, Hu J, Peng Z J Cereb Blood Flow Metab. 2024; 44(9):1565-1576.

PMID: 38459953 PMC: 11418712. DOI: 10.1177/0271678X241238033.

Kinin receptors regulate skeletal muscle regeneration: differential effects for B1 and B2 receptors.

Martins L, Amorim W, Gregnani M, de Carvalho Araujo R, Qadri F, Bader M Inflamm Res. 2023; 72(8):1583-1601.

PMID: 37464053 PMC: 10499706. DOI: 10.1007/s00011-023-01766-4.

Altered Left Ventricular Rat Gene Expression Induced by the Myosin Activator Omecamtiv Mecarbil.

El Oumeiri B, Dewachter L, van de Borne P, Hubesch G, Melot C, Jespers P Genes (Basel). 2023; 14(1).

PMID: 36672863 PMC: 9858687. DOI: 10.3390/genes14010122.

Interrelation among exercise training, cardiac hypertrophy, and tissue kallikrein-kinin system in athlete and non-athlete women.

Heidari B, Zolfaghari M, Khademvatani K, Fattahi A, Zarezadeh R J Cardiovasc Thorac Res. 2022; 14(3):159-165.

PMID: 36398053 PMC: 9617055. DOI: 10.34172/jcvtr.2022.28.