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• W2042582017 abstract "ACTH1–24, its o-nitrophenyl sulfenyl derivative and ACTH11–24 were iodinated by the chloramine T method and purified on carboxymethylcellulose. Enzymatic digestion shows that all the iodine was incorporated in the form of monoiodotyrosine. The three ACTHs bound to adrenal crude membranes (pellet 20,000 g) prepared from normal human, rat and sheep adrenals. In the presence of an excess of membrane protein more than 60% of the radioactivity was bound specifically. The binding of 125I-ACTH1–24 to its adrenal receptor is very rapid; it is temperature dependent, inhibited by ions and by the pancreatic trypsin inhibitor. ACTH1–24 and its o-nitrophenyl sulfenyl derivative inhibited identically the binding of 125I-ACTH1–24. ACTH11–24 and ACTH1–10 were only, respectively, 15% and 6%, as active as ACTH1–24 in displacing the bound 125I-ACTH1–24. The binding of 125I-ACTH11–24 is more inhibited by ACTH1–24 than by ACTH11–24 ACTH1–10 at high concentrations (10−4 M) had no effect. The adenyl cyclase of the same adrenal preparations was stimulated by ACTH1–24; NPS-ACTH1–24 stimulated adenyl cyclase activity but inhibited the action induced by ACTH1–24 in the same way as ACTH11–24 which was without effect on adenyl cyclase. On the other hand, ACTH1–10 stimulated adenyl cyclase activity and its action was additional to ACTH1–24. It can be concluded that the 1–10 N-terminal sequence of ACTH, in addition to being the biological active site of the molecule, contributes to binding and increases the affinity of ACTH for its receptor." @default.
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• W2042582017 date "1974-12-01" @default.
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• W2042582017 title "Interactions of acth with its adrenal receptors: Specific binding of ACTH1–24, its O-nitrophenyl sulfenyl derivative and ACTH11–24" @default.
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• W2042582017 doi "https://doi.org/10.1016/0022-4731(74)90087-9" @default.
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