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A midposition NOTCH3 truncation in inherited cerebral small vessel disease may affect the protein interactome

J Biol Chem .. 2023-01; 
Soo Jung Lee , Xiaojie Zhang , Gang Xu , Jimo Borjigin , Michael M Wang
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Peptide Synthesis All animal experiments were performed by GenScript and reviewed by the GenScript Institutional Animal Care and Use Committee (animal protocol no.: ANT19-005)./Dot blots were performed on spotted peptides (sequences specified in Fig. 2;synthesized by GenScript). Get A Quote
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摘要

Mutations in NOTCH3 underlie cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL), the most common inherited cerebral small vessel disease. Two cleavages of NOTCH3 protein, at Asp80 and Asp121, were previously described in CADASIL pathological samples. Using monoclonal antibodies developed against a NOTCH3 neoepitope, we identified a third cleavage at Asp964 between an Asp-Pro sequence. We characterized the structural requirements for proteolysis at Asp964 and the vascular distribution of the cleavage event. A proteome-wide analysis was performed to find proteins that interact with the cleavage product. Finally, we investigated the biochemical determinants of this... More

关键词

Asp-Pro bond; CADASIL; NOTCH3; nonenzymatic cleavage; protein interactions.