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Literature DB >> 17131193

Molecular cloning, sequence, function and structural basis of human heart 150 kDa oxygen-regulated protein, an ER chaperone.

Abstract

Apoptosis of heart tissues followed by hypoxia and ischemia leads finally to cardiac insufficiency. The full-length coding sequence of 3301 bp including cDNA(s) of the ER chaperone ORP150, which was specifically induced by hypoxia stress, was cloned from human cardiac infarct. Phylogenetic analyses reveal that human heart ORP150 shares a highly conserved N-terminal ATPase domain among its related family members. Moreover, hydropathic profiling reveals that their ca. 70 N-terminal residues and unique C-terminal halves exhibit similar hydropathy profiles among members. These findings suggest that ORP150 is structurally and functionally well conserved in distant species.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 2006 PMID： 17131193 DOI： 10.1007/s10930-006-9038-z

Source DB: PubMed Journal: Protein J ISSN： 1572-3887 Impact factor: 2.371

28 in total

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