High molecular weight kininogen contributes to early mortality and kidney dysfunction in a mouse model of sickle cell disease.

Erica M Sparkenbaugh Malgorzata KasztanMichael W HendersonPatrick EllsworthParker Ross DavisKathryn J WilsonBrandi N Reeves Nigel S Key Sidney Strickland Keith R McCrae David M Pollock Rafal Pawlinski

Published in: Journal of thrombosis and haemostasis : JTH (2020)

We found elevated plasma levels of cleaved HK in sickle patients compared to healthy controls, suggesting ongoing HK activation in SCD. We used bone marrow transplantation to generate wild type and sickle cell mice on a HK-deficient background. We found that short-term HK deficiency attenuated thrombin generation and inflammation in sickle mice at steady state, which was independent of bradykinin signaling. Moreover, long-term HK deficiency attenuates kidney injury, reduces chronic inflammation, and ultimately improves survival of sickle mice.

Keyphrases

wild type
high glucose
sickle cell disease
oxidative stress
bone marrow
high fat diet induced
mouse model
end stage renal disease
chronic kidney disease
prognostic factors
risk factors
cardiovascular events
insulin resistance
cell therapy
free survival