Binding of biotin to streptavidin stabilizes intersubunit salt bridges between Asp61 and His87 at low pH

被引:59
作者
Katz, BA [1 ]
机构
[1] Arris Pharmaceut Corp, S San Francisco, CA 94080 USA
关键词
intersubunit conformational equilibrium; pH-dependent structural changes; shift in pK(a); tetramer stability; strong hydrogen bond;
D O I
10.1006/jmbi.1997.1444
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The remarkable stability of the streptavidin tetramer towards subunit dissociation becomes even greater upon binding of biotin. At two equivalent extensive monomer-monomer interfaces, monomers tightly associate into dimers that in turn associate into the tetramer at a less extensive dimer-dimer interface. To probe the structural basis for the enhancement of the stability of streptavidin by biotin, the crystal structures of apostreptavidin and its complexes with biotin and other small molecule and cyclic peptide ligands were determined and compared at resolutions as high as 1.36 Angstrom over a range of pH values from as low as 1.39. At low pH dramatic changes occur in the conformation and intersubunit hydrogen bonds involving the loop comprising Asp61 to Ser69. The hydrogen-bonded salt bridge between Asp61 O-delta 2 and His87 N-delta 1, observed at higher pH, is replaced with a strong hydrogen bond between Asp61 O-delta 1 and Asn85 O-delta 1. Through crystallography at multiple pH values, the pH where this conformational change occurs, and thus the pK(a) of Asp61, was determined in crystals of space group I222 and/or I4(1)22 of apostreptavidin and complexes. A range in pK, values for Asp61 was observed in these structures, the lowest being 1.78 +/- 0.19 for I222 streptavidin-biotin in 2.9 M (NH4)(2)SO4. At low pH the decrease in pk(a), of Asp61 and preservation of the intersubunit Asp61 O-delta 2-N-delta 1 His87 hydrogen-bonded salt bridge in streptavidin-biotin versus apostreptavidin or streptavidin-peptide complexes is associated with an ordering of the flexible flap comprising residues Ala46 to Glu51, that in turn orders the Arg84 side-chain of a neighboring loop through resulting hydrogen bonds. Ordering of Arg84 in close proximity to the strong intersubunit interface appears to stabilize the conformation associated with the Asp61 O-delta 2-N-delta 1 His87 hydrogen-bonded salt bridge. Thus, in addition to the established role of biotin in tetramer stabilization by direct mediation of intersubunit interactions at the weak interface through contact with Trp120, biotin may enhance tetramer stability at the strong interface more indirectly by ordering loop residues. (C) 1997 Academic Press Limited.
引用
收藏
页码:776 / 800
页数:25
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