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Publication : Cystathionine β-synthase deficiency: different changes in proteomes of thrombosis-resistant Cbs<sup>-/-</sup> mice and thrombosis-prone CBS<sup>-/-</sup> humans.

First Author  Sikora M Year  2020
Journal  Sci Rep Volume  10
Issue  1 Pages  10726
PubMed ID  32612202 Mgi Jnum  J:294188
Mgi Id  MGI:6453196 Doi  10.1038/s41598-020-67672-5
Citation  Sikora M, et al. (2020) Cystathionine beta-synthase deficiency: different changes in proteomes of thrombosis-resistant Cbs(-/-) mice and thrombosis-prone CBS(-/-) humans. Sci Rep 10(1):10726
abstractText  Cystathionine beta-synthase (CBS)-deficient patients are prone to vascular thrombosis. In contrast, Cbs(-/-) mice show no abnormalities in blood coagulation. To identify molecular basis underlying these disparately different thrombotic phenotypes, we analyzed plasma proteomes of Cbs(-/-) vs. Cbs(+/+) mice (8-month-old, 12/group, sex-matched) and CBS(-/-) vs. CBS(+/+) humans (37 +/- 7-year-old, 10-14/group, sex-matched) using label-free mass spectrometry. We identified 117 and 41 differentiating plasma proteins in Cbs(-/-) mice and CBS(-/-) humans, respectively. Twenty-one proteins were shared between CBS(-/-) humans and Cbs(-/-) mice, with sixteen changed in the opposite direction. Proteins involved in blood coagulation and complement/coagulation cascades represented a greater fraction of the differentiating proteins in CBS(-/-) patients (51%) than in Cbs(-/-) mice (21%). Top canonical pathways, identified by Ingenuity Pathways Analysis, such as LXR/RXR, FXR/RXR activation (- log[P-value] = 30-31) and atherosclerosis signaling (- log[P-value] = 10-11) were similarly affected in Cbs(-/-) mice and CBS(-/-) humans. The Coagulation System was affected stronger in CBS(-/-) humans than in Cbs(-/-) mice (- log[P-value] = 15 vs. 10, respectively) while acute phase response and complement system were affected stronger in Cbs(-/-) mice (- log[P-value] = 33 and 22, respectively) than in humans (- log[P-value] = 22 and 6, respectively). Other pathways, including IL-7 signaling and B cell development were affected only in Cbs(-/-) mice. Taken together, our findings suggest that differences in these processes, in particular in the Coagulation System, could account for the thrombotic phenotype in CBS(-/-) patients and the absence of thrombosis in Cbs(-/-) mice. Overall, our findings suggest that Cbs(-/-) mice have a better adaptive response to protect from prothrombotic effects of hyperhomocysteinemia than CBS(-/-) humans.
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