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Functional and structural analyses of N‐ acylsulfonamide‐linked dinucleoside inhibitors of RNase A
Author(s) -
Thiyagarajan Nethaji,
Smith Bryan D.,
Raines Ronald T.,
Acharya K. Ravi
Publication year - 2011
Publication title -
the febs journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.981
H-Index - 204
eISSN - 1742-4658
pISSN - 1742-464X
DOI - 10.1111/j.1742-4658.2010.07976.x
Subject(s) - rnase p , nucleic acid , chemistry , stereochemistry , hydrogen bond , enzyme , accession number (library science) , biochemistry , molecule , rna , organic chemistry , genbank , gene
Molecular probes are useful for both studying and controlling the functions of enzymes and other proteins. The most useful probes have high affinity for their target, along with small size and resistance to degradation. Here, we report on new surrogates for nucleic acids that fulfill these criteria. Isosteres in which phosphoryl [R–O–P(O 2 − )–O–R′] groups are replaced with N ‐acylsulfonamidyl [R–C(O)–N − –S(O 2 )–R′] or sulfonimidyl [R–S(O 2 )–N − –S(O 2 )–R′] groups increase the number of nonbridging oxygens from two (phosphoryl) to three ( N ‐acylsulfonamidyl) or four (sulfonimidyl). Six such isosteres were found to be more potent inhibitors of catalysis by bovine pancreatic RNase A than are parent compounds containing phosphoryl groups. The atomic structures of two RNase A· N ‐acylsulfonamide complexes were determined at high resolution by X‐ray crystallography. The N ‐acylsulfonamidyl groups were observed to form more hydrogen bonds with active site residues than did the phosphoryl groups in analogous complexes. These data encourage the further development and use of N ‐acylsulfonamides and sulfonimides as antagonists of nucleic acid‐binding proteins. Database
Structural data for the two RNase A complexes are available in the Protein Data Bank under accession numbers 2xog and 2xoi