| Literature DB >> 17525278 |
Xiao Z Shen1, Ping Li, Daiana Weiss, Sebastien Fuchs, Hong D Xiao, Jon A Adams, Ifor R Williams, Mario R Capecchi, W Robert Taylor, Kenneth E Bernstein.
Abstract
Angiotensin-converting enzyme (ACE) is a peptidase responsible for the cleavage of angiotensin I and several other peptides. Here, gene targeting was used to switch control of the ACE locus from the endogenous promoter to the macrophage-specific c-fms promoter. Challenge of these mice, called ACE 10/10, with the aggressive mouse melanoma cell line B16 showed that they are remarkably resistant to tumor growth. Tumor resistance was seen after challenge with different melanoma cell lines and in mice with different genetic backgrounds. Histological study of the tumors that did grow in ACE 10/10 mice showed an enhanced inflammatory response. ACE 10/10 mice had increased numbers of tumor epitope-specific CD8(+) T cells after challenge with melanoma or lymphoma. ACE 10/10 macrophages showed increased production of interleukin-12 and nitric oxide but reduced interleukin-10. Engraftment of wild-type mice with ACE 10/10 bone marrow transferred B16 tumor resistance. Injection of B16 tumors with ACE 10/10 macrophages also reduced tumor growth. ACE 10/10 mice may define a new means of enhancing the immune response, which may be potentially useful in several human clinical situations.Entities:
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Year: 2007 PMID: 17525278 PMCID: PMC1899454 DOI: 10.2353/ajpath.2007.061205
Source DB: PubMed Journal: Am J Pathol ISSN: 0002-9440 Impact factor: 4.307