New melanocortin-like peptide of can suppress inflammation via the mammalian melanocortin-1 receptor (MC1R): possible endocrine-like function for microbes of the gut.
| Citation | Qiang, Xiaoling, et al. “New Melanocortin-Like Peptide of Can Suppress Inflammation via the Mammalian Melanocortin-1 Receptor (MC1R): Possible Endocrine-Like Function for Microbes of the Gut”. 2017. NPJ Biofilms and Microbiomes, vol. 3, 2017, p. 31.  | 
       
| Center | Albert Einstein College of Medicine | 
| Author | Xiaoling Qiang, Anthony S Liotta, Joseph Shiloach, J C Gutierrez, Haichao Wang, Mahendar Ochani, Kanta Ochani, Huan Yang, Aviva Rabin, Derek LeRoith, Maxine A Lesniak, Markus Böhm, Christian Maaser, Klaus Kannengiesser, Mark Donowitz, Shervin Rabizadeh, Christopher J Czura, Kevin J Tracey, Mark Westlake, Aida Zarfeshani, Syed F Mehdi, Ann Danoff, Xueliang Ge, Suparna Sanyal, Gary J Schwartz, Jesse Roth | 
| Abstract | 
   releases a 33 amino acid peptide melanocortin-like peptide of (MECO-1) that is identical to the C-terminus of the elongation factor-G (EF-G) and has interesting similarities to two prominent mammalian melanocortin hormones, alpha-melanocyte-stimulating hormone (alpha-MSH) and adrenocorticotropin (ACTH). Note that MECO-1 lacks HFRW, the common pharmacophore of the known mammalian melanocortin peptides. MECO-1 and the two hormones were equally effective in severely blunting release of cytokines (HMGB1 and TNF) from macrophage-like cells in response to (i) endotoxin (lipopolysaccharide) or (ii) pro-inflammatory cytokine HMGB-1. The in vitro anti-inflammatoty effects of MECO-1 and of alpha-MSH were abrogated by (i) antibody against melanocortin-1 receptor (MC1R) and by (ii) agouti, an endogenous inverse agonist of MC1R. In vivo MECO-1 was even more potent than alpha-MSH in rescuing mice from death due to (i) lethal doses of LPS endotoxin or (ii) cecal ligation and puncture, models of sterile and infectious sepsis, respectively.  | 
        
| Year of Publication | 
   2017 
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| Journal | 
   NPJ biofilms and microbiomes 
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| Volume | 
   3 
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| Number of Pages | 
   31 
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| Date Published | 
   12/2017 
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| ISSN Number | 
   2055-5008 
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| DOI | 
   10.1038/s41522-017-0039-9 
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| Alternate Journal | 
   NPJ Biofilms Microbiomes 
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| PMCID | 
   PMC5684143 
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| PMID | 
   29152323 
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