2018
DOI: 10.1021/acs.biochem.8b00418
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Mapping Functional Substrate–Enzyme Interactions in the pol β Active Site through Chemical Biology: Structural Responses to Acidity Modification of Incoming dNTPs

Abstract: We report high-resolution crystal structures of DNA polymerase (pol) β in ternary complex with a panel of incoming dNTPs carrying acidity-modified 5'-triphosphate groups. These novel dNTP analogues have a variety of halomethylene substitutions replacing the bridging oxygen between Pβ and Pγ of the incoming dNTP, whereas other analogues have alkaline substitutions at the bridging oxygen. Use of these analogues allows the first systematic comparison of effects of 5'-triphosphate acidity modification on active si… Show more

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Cited by 12 publications
(36 citation statements)
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“…In general, the ternary complex crystal structures of pol β with the various dNTP analogues were found to be similar to the reference structure with a normal incoming dNTP. This observation facilitated interpretations regarding the acidity modification effects on the nucleotidyl transferase reaction versus other influences such as conformational effects . Interestingly, an exception to the structural conservation was found with one type of incoming dNTP analogue, the dATP analogue with the CF 2 group substitution.…”
mentioning
confidence: 87%
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“…In general, the ternary complex crystal structures of pol β with the various dNTP analogues were found to be similar to the reference structure with a normal incoming dNTP. This observation facilitated interpretations regarding the acidity modification effects on the nucleotidyl transferase reaction versus other influences such as conformational effects . Interestingly, an exception to the structural conservation was found with one type of incoming dNTP analogue, the dATP analogue with the CF 2 group substitution.…”
mentioning
confidence: 87%
“…This observation facilitated interpretations regarding the acidity modification effects on the nucleotidyl transferase reaction versus other influences such as conformational effects. 23 Interestingly, an exception to the structural conservation was found with one type of incoming dNTP analogue, the dATP analogue with the CF 2 group substitution. In this case, the CF 2 group appeared to introduce strain into the structure preventing the open to closed conformational change and distorting the position of α-helix N in the active site.…”
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confidence: 99%
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“…Polymerase structures also have significant value in the engineering process, particularly from related structures harbouring a range of substrates, sampling mismatches [47,48], unnatural bases [49] and triphosphate analogues [50]. Those "families" of structures give a very detailed knowledge of spatial constraints that can affect polymerase function.…”
Section: Future Of Polymerase Engineeringmentioning
confidence: 99%