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A novel peptide interferes with Mycobacterium tuberculosis virulence and survival.

FEBS Open Bio. 2014; 
Samuchiwal SK, Tousif S, Singh DK, Kumar A, Ghosh A, Bhalla K, Prakash P, Kumar S, Trivedi AC, Bhattacharyya M, Das G, Ranganathan A.
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Peptide Synthesis … SL3-His 6X peptide (GenScript, Hong Kong) was added to 7H9 medium exogenously (H37Rv + SL3) at a final concentration of 10 μg/ml. ΔRD1, H37Rv + DL1 (addition of an unrelated peptide at same concentration; sequence provided in Supplementary Fig … Get A Quote

摘要

Tuberculosis (TB) is a huge global burden, with new and resistant strains emerging at an alarming rate, necessitating an urgent need for a new class of drug candidates. Here, we report that SL3, a novel 33-amino acid peptide, causes debilitating effects on mycobacterial morphology. Treatment with SL3 drastically inhibits the growth of Mycobacterium tuberculosis in vitro as well as in a pre-clinical mouse model for M.tb infection. Microarray analysis of SL3-expressing strain demonstrates wide-scale transcriptional disruption in M.tb. We therefore believe that SL3 and similar peptides may herald a new approach towards discovering new molecules for TB therapy.

关键词

AMADID, agilent microarray design identifiers; Antimycobacterial peptides; CFU, colony forming units; ESAT6; MOI, multiplicity of infection; Mycobacterium tuberculosis; Protein–protein interaction; RD1, region of difference 1