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Analysis of spinal and muscle pathology in transgenic mice overexpressing wild-type and ALS-linked mutant MATR3.

Acta Neuropathol Commun. 2018; 
Moloney C,, Rayaprolu S,, Howard J,, Fromholt S,, Brown H,, Collins M,, Cabrera M,, Duffy C,, Siemienski Z,, Miller D,, Borchelt DR,,, Lewis J,,.
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Catalog Antibody The PCR products were purified using a Monarch PCR & DNA cleanup kit (New England BioLabs catalog #T1030S) and then the purified PCR products were sent to GenScript for sequencing (Additional file 1: Table S1, asterisk) using the following primer which would allow for unambiguous iden- tification of the sequences encoding both S85 and F115 positions: (antisense) 5’ CCATAACTCAAGGTAGAGCCT TCTTCAGTTC 3′. Get A Quote

摘要

Mutations in MATR3 have been associated with amyotrophic lateral sclerosis (ALS) as well as a form of distal myopathy termed vocal cord pharyngeal distal myopathy (VCPDM). To begin to understand how mutations in MATR3 may cause disease, here we provide initial characterization of transgenic (Tg) mice expressing human wild-type (WT) MATR3 (MATR3WT) and ALS-mutant F115C MATR3 (MATR3F115C) proteins under the control of the mouse prion promoter (MoPrP). For each construct, we established multiple independent lines of mice that stably transmitted the transgene. Unexpectedly, for all stably-transmitting lines examined, MATR3 transgenic mRNA expression was more robust in muscle, with minimal expression in spinal cord.... More

關鍵詞

ALS; Distal myopathy; MATR3; Transgenic mouse model
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