The protein that binds to DNA base J in trypanosomatids has features of a thymidine hydroxylase |
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Authors: | Yu Zhong Genest Paul-André ter Riet Bas Sweeney Kate DiPaolo Courtney Kieft Rudo Christodoulou Evangelos Perrakis Anastassis Simmons Jana M Hausinger Robert P van Luenen Henri G A M Rigden Daniel J Sabatini Robert Borst Piet |
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Affiliation: | Division of Molecular Biology and Centre of Biomedical Genetics, The Netherlands Cancer Institute, Amsterdam, The Netherlands. |
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Abstract: | Trypanosomatids contain an unusual DNA base J (beta-d-glucosylhydroxymethyluracil), which replaces a fraction of thymine in telomeric and other DNA repeats. To determine the function of base J, we have searched for enzymes that catalyze J biosynthesis. We present evidence that a protein that binds to J in DNA, the J-binding protein 1 (JBP1), may also catalyze the first step in J biosynthesis, the conversion of thymine in DNA into hydroxymethyluracil. We show that JBP1 belongs to the family of Fe(2+) and 2-oxoglutarate-dependent dioxygenases and that replacement of conserved residues putatively involved in Fe(2+) and 2-oxoglutarate-binding inactivates the ability of JBP1 to contribute to J synthesis without affecting its ability to bind to J-DNA. We propose that JBP1 is a thymidine hydroxylase responsible for the local amplification of J inserted by JBP2, another putative thymidine hydroxylase. |
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