Roberts Marnie S, Woods Alison J, Dale Trevor C, Van Der Sluijs Peter, Norman Jim C
Department of Biochemistry, University of Leicester, Leicester LE1 7RH, United Kingdom.
Mol Cell Biol. 2004 Feb;24(4):1505-15. doi: 10.1128/MCB.24.4.1505-1515.2004.
Protein kinase B (PKB)/Akt is known to promote cell migration, and this may contribute to the enhanced invasiveness of malignant cells. To elucidate potential mechanisms by which PKB/Akt promotes the migration phenotype, we have investigated its role in the endosomal transport and recycling of integrins. Whereas the internalization of alpha v beta 3 and alpha 5 beta 1 integrins and their transport to the recycling compartment were independent of PKB/Akt, the return of these integrins (but not internalized transferrin) to the plasma membrane was regulated by phosphatidylinositol 3-kinases and PKB/Akt. The blockade of integrin recycling and cell spreading on integrin ligands effected by inhibition of PKB/Akt was reversed by inhibition of glycogen synthase kinase 3 (GSK-3). Moreover, expression of nonphosphorylatable active GSK-3 beta mutant GSK-3 beta-A9 suppressed recycling of alpha 5 beta 1 and alpha v beta 3 and reduced cell spreading on ligands for these integrins, indicating that PKB/Akt promotes integrin recycling by phosphorylating and inactivating GSK-3. We propose that the ability of PKB/Akt to act via GSK-3 to promote the recycling of matrix receptors represents a key mechanism whereby integrin function and cell migration can be regulated by growth factors.
蛋白激酶B(PKB)/Akt已知可促进细胞迁移,这可能导致恶性细胞侵袭性增强。为了阐明PKB/Akt促进迁移表型的潜在机制,我们研究了其在内体运输和整合素循环利用中的作用。虽然αvβ3和α5β1整合素的内化及其向循环区室的运输与PKB/Akt无关,但这些整合素(而非内化的转铁蛋白)返回质膜的过程受磷脂酰肌醇3激酶和PKB/Akt的调节。通过抑制糖原合酶激酶3(GSK-3)可逆转抑制PKB/Akt所导致的整合素循环利用受阻以及细胞在整合素配体上的铺展。此外,不可磷酸化的活性GSK-3β突变体GSK-3β-A9的表达抑制了α5β1和αvβ3的循环利用,并减少了细胞在这些整合素配体上的铺展,这表明PKB/Akt通过磷酸化并使GSK-3失活来促进整合素的循环利用。我们提出,PKB/Akt通过GSK-3促进基质受体循环利用的能力代表了一种关键机制,借此生长因子可调节整合素功能和细胞迁移。
