RRC ID 38170
著者 Kunoh T, Noda T, Koseki K, Sekigawa M, Takagi M, Shin-ya K, Goshima N, Iemura S, Natsume T, Wada S, Mukai Y, Ohta S, Sasaki R, Mizukami T.
タイトル A novel human dynactin-associated protein, dynAP, promotes activation of Akt, and ergosterol-related compounds induce dynAP-dependent apoptosis of human cancer cells.
ジャーナル Mol Cancer Ther
Abstract There are several human genes that may encode proteins whose functions remain unknown. To find clues to their functions, we used the mutant yeast defective in Mad2, a component of the spindle checkpoint complex. Phenotypes that were provoked by the expression of a human C18orf26 protein in the mutant yeast encouraged further characterization of this protein in human cells. This protein was designated dynAP (dynactin-associated protein) because of its interaction with dynactin subunits that comprised a microtubule-based motor protein complex. The dynAP is a transmembrane protein localizing to Golgi apparatus and plasma membrane in a microtubule-dependent manner. This protein was expressed in half of human cancer cell lines but barely in normal human fibroblasts tested. The SV40-transformed fibroblasts expressed dynAP. Importantly, the expression of dynAP activated Akt (also known as protein kinase B) by promoting Ser⁴⁷³ phosphorylation required for the full activation, whereas knockdown of dynAP abolished this activation. The ergosterol-related compounds identified by the yeast cell-based high-throughput screen abrogated activation of Akt and induced apoptosis in a dynAP-dependent manner. We propose a possible advantage of dynAP expression in cancer cells; the survival of cancer cells that express dynAP is supported by dynAP-induced activation of Akt, sustaining high rates of proliferation. The inactivation of dynAP by the selected compounds nullifies this advantage, and thereby, the apoptotic machinery is allowed to operate. Taken together, dynAP can be a new target for cancer therapy, and the selected chemicals are useful for developing a new class of anticancer drugs.
巻・号 9(11)
ページ 2934-42
公開日 2010-11-1
DOI 10.1158/1535-7163.MCT-10-0730
PII 1535-7163.MCT-10-0730
PMID 20978158
MeSH Apoptosis / drug effects* Apoptosis / genetics Caco-2 Cells Cells, Cultured Drug Screening Assays, Antitumor Dynactin Complex Enzyme Activation Ergosterol / analogs & derivatives* Ergosterol / pharmacology HCT116 Cells HeLa Cells Hep G2 Cells Humans Membrane Proteins Microtubule-Associated Proteins / genetics Microtubule-Associated Proteins / metabolism Microtubule-Associated Proteins / physiology* Neoplasms / genetics Neoplasms / metabolism Neoplasms / pathology* Oncogene Protein v-akt / metabolism* Organisms, Genetically Modified Protein Binding Sterols / pharmacology* Up-Regulation Yeasts
IF 5.615
引用数 7
WOS 分野 ONCOLOGY
リソース情報
ヒト・動物細胞 WI-38(RCB0704)