Concanamycin a, the specific inhibitor of V-ATPases, binds to the Vo subunit c

被引:224
作者
Huss, M [1 ]
Ingenhorst, G [1 ]
König, S [1 ]
Gassel, M [1 ]
Dröse, S [1 ]
Zeeck, A [1 ]
Altendorf, K [1 ]
Wieczorek, H [1 ]
机构
[1] Univ Osnabruck, Fachbereich Biol Chem, Abt Tierphysiol, D-49069 Osnabruck, Germany
关键词
D O I
10.1074/jbc.M207345200
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
Vacuolar-type ATPase (V-ATPase) purified from the midgut of the tobacco hornworm Manduca sexta is inhibited 50% by 10 nm of the plecomacrolide concanamycin A, the specific inhibitor of V-ATPases. To determine the binding site(s) of that antibiotic in the enzyme complex, labeling with the semisynthetic 9-O-[p-(trifluoroethyldiazirinyl)-benzoyl]-21,23-dideoxy-23-[I-125]iodo-concanolide A (J-concanolide A) was performed, which still inhibits the V-ATPase 50% at a concentration of 15-20 mum. Upon treatment with UV light, a highly reactive carbene is generated from this concanamycin derivative, resulting in the formation of a covalent bond to the enzyme. In addition, the radioactive tracer 1251 makes the detection of the labeled subunit(s) feasible. Treatment of the V-1/V-o holoenzyme, the V-o complex, and the V-ATPase containing goblet cell apical membranes with concanolide resulted in the labeling of only the proteolipid, subunit c, of the proton translocating V-o complex. Binding of J-concanolide A to subunit c was prevented in a concentration-dependent manner by concanamycin A, indicating that labeling was specific. Binding was also prevented by the plecomacrolides bafilomycin A(1) and B-1 respectively, but not by the benzolactone enamide salicylihalamide, a member of a novel class of V-ATPase inhibitors.
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页码:40544 / 40548
页数:5
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