SURF-1 Background Information The SURF-1 protein demonstrates a vital role in the assembly of complex IV (CIV or COX) of the mitochondrial respiratory chain. Expressed in the inner mitochondrial membrane, mutations of the SURF-1 gene generally cause cytochrome c oxidase complex IV deficiency. Shortage of complex IV leads to Leigh syndrome, a severe neurological disorder. Leigh syndrome patients are usually subject to rapidly progressive encephalopathy, characterized by necrotic lesions in subcortical brain regions. SURF-1 mutations correlate to high post-implantation embryonic lethality as well as early-onset mortality of post-natal individuals. Considerable deficit in muscle strength and motor performance is also a profound and isolated defect of SURF-1 activity in skeletal muscle and liver. Heart, brain and skeletal muscle morphological abnormalities frequently occur due to SURF-1 mutations.
SURF-1 (21H2)
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SURF-1 (21H2): sc-65245. Western blot analysis of SURF-1 expression in human heart (A) and mouse liver (B) tissue extracts.
SURF-1 (21H2): sc-65245. Western blot analysis of SURF-1 expression in non-transfected: sc-117750 (A) and SURF-1 transfected: sc-110127 (B) CHO whole cell lysate.
SURF-1 (21H2): sc-65245. Western blot analysis of SURF-1 expression in HeLa whole cell lysate.
SURF-1 (21H2): sc-65245. Western blot analysis of SURF-1 expression in non-transfected: sc-117752 (A) and human SURF-1 transfected: sc-110725 (B) 293T whole cell lysates.
