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MUTATIONAL ANALYSIS OF THE RICINUS LECTIN B-CHAINS - GALACTOSE-BINDING ABILITY OF THE 2-GAMMA SUBDOMAIN OF RICINUS-COMMUNIS AGGLUTININ B-CHAIN
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UNSPECIFIED (1995) MUTATIONAL ANALYSIS OF THE RICINUS LECTIN B-CHAINS - GALACTOSE-BINDING ABILITY OF THE 2-GAMMA SUBDOMAIN OF RICINUS-COMMUNIS AGGLUTININ B-CHAIN. JOURNAL OF BIOLOGICAL CHEMISTRY, 270 (35). pp. 20292-20297. ISSN 0021-9258.
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Abstract
Ricin B-chain (RTB) is a galactose-specific lectin that folds into two globular domains, each of which binds a single galactoside. The two binding sites are structurally similar and both contain a conserved tripeptide kink and an aromatic residue that comprises a sugar-binding platform. Whereas the critical RTB residues implicated in lectin activity are conserved in domain 1 of Ricinus communis agglutinin (RCA) B chain, the sugar platform aromatic residue Tyr-248 present in domain 2 of RTB is replaced by His in RCA B-chain. In this study, key residues in the vicinity of the binding sites of the Ricinus lectin B chains were altered by site directed mutagenesis. The recombinant B-chains were produced in Xenopus oocytes in soluble, stable, and core-glycosylated forms. Both sites of RCA B chain must be simultaneously modified in order to abolish lectin activity, indicating the presence of two independent, functional binding sites/molecule. Activity associated with the domain 2 site of RCA B chain is abrogated by the conversion of Trp-258 to Ser. Moreover, the domain 2 site appears responsible for a weak binding interaction of recombinant RCA B-chain with GalNAc, not observed with native tetrameric RCA. Finally, the introduction of His at position 248 of RTB severely disrupts but does not abolish GalNAc binding.
Item Type: | Journal Article | ||||
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Subjects: | Q Science > QD Chemistry | ||||
Journal or Publication Title: | JOURNAL OF BIOLOGICAL CHEMISTRY | ||||
Publisher: | AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC | ||||
ISSN: | 0021-9258 | ||||
Official Date: | 1 September 1995 | ||||
Dates: |
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Volume: | 270 | ||||
Number: | 35 | ||||
Number of Pages: | 6 | ||||
Page Range: | pp. 20292-20297 | ||||
Publication Status: | Published |
Data sourced from Thomson Reuters' Web of Knowledge
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