Okumura Takashi, Sasamura Takeshi, Inatomi Momoko, Hozumi Shunya, Nakamura Mitsutoshi, Hatori Ryo, Taniguchi Kiichiro, Nakazawa Naotaka, Suzuki Emiko, Maeda Reo, Yamakawa Tomoko, Matsuno Kenji
Department of Biological Science and Technology, Tokyo University of Science, Tokyo 125-1500, Japan.
Department of Biological Science and Technology, Tokyo University of Science, Tokyo 125-1500, Japan Department of Biological Sciences, Graduate School of Science, Osaka University, Osaka 560-0043, Japan.
Genetics. 2015 Apr;199(4):1183-99. doi: 10.1534/genetics.115.174698. Epub 2015 Feb 6.
The class I myosin genes are conserved in diverse organisms, and their gene products are involved in actin dynamics, endocytosis, and signal transduction. Drosophila melanogaster has three class I myosin genes, Myosin 31DF (Myo31DF), Myosin 61F (Myo61F), and Myosin 95E (Myo95E). Myo31DF, Myo61F, and Myo95E belong to the Myosin ID, Myosin IC, and Myosin IB families, respectively. Previous loss-of-function analyses of Myo31DF and Myo61F revealed important roles in left-right (LR) asymmetric development and enterocyte maintenance, respectively. However, it was difficult to elucidate their roles in vivo, because of potential redundant activities. Here we generated class I myosin double and triple mutants to address this issue. We found that the triple mutant was viable and fertile, indicating that all three class I myosins were dispensable for survival. A loss-of-function analysis revealed further that Myo31DF and Myo61F, but not Myo95E, had redundant functions in promoting the dextral LR asymmetric development of the male genitalia. Myo61F overexpression is known to antagonize the dextral activity of Myo31DF in various Drosophila organs. Thus, the LR-reversing activity of overexpressed Myo61F may not reflect its physiological function. The endogenous activity of Myo61F in promoting dextral LR asymmetric development was observed in the male genitalia, but not the embryonic gut, another LR asymmetric organ. Thus, Myo61F and Myo31DF, but not Myo95E, play tissue-specific, redundant roles in LR asymmetric development. Our studies also revealed differential colocalization of the class I myosins with filamentous (F)-actin in the brush border of intestinal enterocytes.
I类肌球蛋白基因在多种生物中保守,其基因产物参与肌动蛋白动力学、内吞作用和信号转导。黑腹果蝇有三个I类肌球蛋白基因,即肌球蛋白31DF(Myo31DF)、肌球蛋白61F(Myo61F)和肌球蛋白95E(Myo95E)。Myo31DF、Myo61F和Myo95E分别属于肌球蛋白ID、肌球蛋白IC和肌球蛋白IB家族。先前对Myo31DF和Myo61F的功能丧失分析分别揭示了它们在左右(LR)不对称发育和肠上皮细胞维持中的重要作用。然而,由于潜在的冗余活性,很难在体内阐明它们的作用。在这里,我们生成了I类肌球蛋白双突变体和三突变体来解决这个问题。我们发现三突变体是有活力且可育的,这表明所有这三种I类肌球蛋白对于生存都是非必需的。功能丧失分析进一步表明,Myo31DF和Myo61F,而非Myo95E,在促进雄性生殖器的右旋LR不对称发育中具有冗余功能。已知Myo61F的过表达会拮抗Myo31DF在各种果蝇器官中的右旋活性。因此,过表达的Myo61F的LR反转活性可能无法反映其生理功能。在雄性生殖器中观察到了Myo61F在促进右旋LR不对称发育中的内源性活性,但在另一个LR不对称器官胚胎肠道中未观察到。因此,Myo61F和Myo31DF,而非Myo95E,在LR不对称发育中发挥组织特异性的冗余作用。我们的研究还揭示了I类肌球蛋白与肠上皮细胞刷状缘中的丝状(F)肌动蛋白的不同共定位情况。