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Arsenite Exposure Displaces Zinc from ZRANB2 Leading to Altered Splicing

Chem Res Toxicol. 2020; 
Mayukh Banerjee, Ana P Ferragut Cardoso, Angeliki Lykoudi, Daniel W Wilkey, Jianmin Pan, Walter H Watson, Nichola C Garbett, Shesh N Rai, Michael L Merchant, J Christopher States
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Peptide Synthesis … Guidelines for the Use of Chemical Carcinogens. Chemicals. Synthetic apo-peptides corresponding to the two ZRANB2 zfms (For sequences, see Table 1) were obtained from GenScript Corp. (Piscataway, NJ, USA) at a purity >95%. Zinc … Get A Quote

摘要

Exposure to arsenic, a class I carcinogen, affects 200 million people globally. Skin is the major target organ, but the molecular etiology of arsenic-induced skin carcinogenesis remains unclear. Arsenite (As)-induced disruption of alternative splicing could be involved, but the mechanism is unknown. Zinc finger proteins play key roles in alternative splicing. As can displace zinc (Zn) from C3H1 and C4 zinc finger motifs (zfm's), affecting protein function. ZRANB2, an alternative splicing regulator with two C4 zfm's integral to its structure and splicing function, was chosen as a candidate for this study. We hypothesized that As could displace Zn from ZRANB2, altering its structure, expression, and splicing func... More

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