Literature DB >> 27863446

Glutathione transferase P1-1 as an arsenic drug-sequestering enzyme.

Lorien J Parker1,2, Alessio Bocedi3, David B Ascher1, Jade B Aitken4, Hugh H Harris5, Mario Lo Bello6, Giorgio Ricci3, Craig J Morton1, Michael W Parker1,2.   

Abstract

Arsenic-based compounds are paradoxically both poisons and drugs. Glutathione transferase (GSTP1-1) is a major factor in resistance to such drugs. Here we describe using crystallography, X-ray absorption spectroscopy, mutagenesis, mass spectrometry, and kinetic studies how GSTP1-1 recognizes the drug phenylarsine oxide (PAO). In conditions of cellular stress where glutathione (GSH) levels are low, PAO crosslinks C47 to C101 of the opposing monomer, a distance of 19.9 Å, and causes a dramatic widening of the dimer interface by approximately 10 Å. The GSH conjugate of PAO, which forms rapidly in cancerous cells, is a potent inhibitor (Ki  = 90 nM) and binds as a di-GSH complex in the active site forming part of a continuous network of interactions from one active site to the other. In summary, GSTP1-1 can detoxify arsenic-based drugs by sequestration at the active site and at the dimer interface, in situations where there is a plentiful supply of GSH, and at the reactive cysteines in conditions of low GSH.
© 2016 The Protein Society.

Entities:  

Keywords:  X-ray crystallography; arsenic; glutathione transferases; inhibitors; resistance

Mesh:

Substances:

Year:  2016        PMID: 27863446      PMCID: PMC5275733          DOI: 10.1002/pro.3084

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


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