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Crystal structure of the N domain of human somatic angiotensin I-converting enzyme provides a structural basis for domain-specific inhibitor design. | LitMetric

AI Article Synopsis

  • Human somatic angiotensin I-converting enzyme (sACE) is vital for regulating blood pressure and is a target for cardiovascular and renal disease treatments.
  • The enzyme consists of two linked metallopeptidase domains (N and C), which both process the peptides angiotensin I and bradykinin, but they interact differently with various substrates and inhibitors.
  • This study reveals the crystal structure of the N domain of sACE, with and without the drug lisinopril, enhancing our understanding of domain functionality and aiding the development of new, more targeted ACE inhibitors.

Article Abstract

Human somatic angiotensin I-converting enzyme (sACE) is a key regulator of blood pressure and an important drug target for combating cardiovascular and renal disease. sACE comprises two homologous metallopeptidase domains, N and C, joined by an inter-domain linker. Both domains are capable of cleaving the two hemoregulatory peptides angiotensin I and bradykinin, but differ in their affinities for a range of other substrates and inhibitors. Previously we determined the structure of testis ACE (C domain); here we present the crystal structure of the N domain of sACE (both in the presence and absence of the antihypertensive drug lisinopril) in order to aid the understanding of how these two domains differ in specificity and function. In addition, the structure of most of the inter-domain linker allows us to propose relative domain positions for sACE that may contribute to the domain cooperativity. The structure now provides a platform for the design of "domain-specific" second-generation ACE inhibitors.

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Source
http://dx.doi.org/10.1016/j.jmb.2006.01.048DOI Listing

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