Selective Inhibition of Bacterial Topoisomerase I by alkynyl-bisbenzimidazoles

Nihar Ranjan; Geraldine Fulcrand; Ada King; Joseph Brown; Xiuping Jiang; Fenfei Leng; Dev P Arya

doi:10.1039/C4MD00140K

Selective Inhibition of Bacterial Topoisomerase I by alkynyl-bisbenzimidazoles

Medchemcomm. 2014 Jun 1;5(6):816-825. doi: 10.1039/C4MD00140K.

Authors

Nihar Ranjan¹, Geraldine Fulcrand², Ada King³, Joseph Brown⁴, Xiuping Jiang⁴, Fenfei Leng², Dev P Arya⁵

Affiliations

¹ Department of Chemistry, Clemson University, Clemson, South Carolina, Unite States 29634.
² Department of Chemistry and Biochemistry, Florida International University, Miami, Florida 33199 (Unite States).
³ NUBAD, LLC, 900 B West Faris Road, Greenville, South Carolina 29605.
⁴ Department of Biological Sciences, Clemson University, Clemson, South Carolina 29634.
⁵ Department of Chemistry, Clemson University, Clemson, South Carolina, Unite States 29634 ; NUBAD, LLC, 900 B West Faris Road, Greenville, South Carolina 29605.

Abstract

Hoechst dyes are well known DNA binders that non-selectively inhibit the function of mammalian topoisomerase I and II. Herein, we show that Hoechst 33258 based bisbenzimidazoles (DPA 151-154), containing a terminal alkyne, are effective and selective inhibitors of E. coli. topoisomerase I. These bisbenzimidazoles displayed topoisomerase I inhibition much better than Hoechst 33342 or Hoechst 33258 with IC50 values in the range of 2.47-6.63 μM. Bisbenzimidazoles DPA 151-154 also display selective inhibition of E. coli. topoisomerase I over DNA gyrase and Human topoisomerases I and II, and effectively inhibit bacterial growth.

Abstract

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