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Cells respond to and bind countin, a component of a multisubunit cell number counting factor.

作者信息

Gao Tong, Ehrenman Karen, Tang Lei, Leippe Matthias, Brock Debra A, Gomer Richard H

机构信息

Howard Hughes Medical Institute, Rice University, Houston, Texas 77005-1892, USA.

出版信息

J Biol Chem. 2002 Sep 6;277(36):32596-605. doi: 10.1074/jbc.M203075200. Epub 2002 Jun 17.

Abstract

In Dictyostelium discoideum counting factor (CF), a secreted approximately 450-kDa complex of polypeptides, inhibits group and fruiting body size. When the gene encoding countin (a component of CF) was disrupted, cells formed large groups. We find that recombinant countin causes developing cells to form small groups, with an EC(50) of approximately 3 ng/ml, and affects cAMP signal transduction in the same manner as semipurified CF. Recombinant countin increases cell motility, decreases cell-cell adhesion, and regulates gene expression in a manner similar to the effect of CF. However, countin does not decrease adhesion or group size to the extent that semipurified CF does. A 1-min exposure of developing cells to countin causes an increase in F-actin polymerization and myosin phosphorylation and a decrease in myosin polymerization, suggesting that countin activates a rapid signal transduction pathway. (125)I-Labeled countin has countin bioactivity, and binding experiments suggest that vegetative and developing cells have approximately 53 cell-surface sites that bind countin with a K(D) of approximately 1.5 ng/ml or 60 pm. We hypothesize that countin regulates cell development through the same pathway as CF and that other proteins within the complex may modify the activity of countin and/or have independent size-regulating activities.

摘要

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