Neurodevelopment requires precise translational control, the disruption of which is implicated in various neurological disorders, including developmental delays, intellectual disability, and microcephaly. We report a novel role for the Drosophila CPEB-family protein Orb2, a translational regulator, in controlling brain size in a dose dependent manner. Loss of orb2 results in larval brain hypotrophy, whereas orb2 overexpression causes brain overgrowth. We demonstrate that orb2 is required for neural stem cell development from embryonic stages through larval neurogenesis. Structure-function analysis reveals that Orb2 RNA-binding activity promotes brain growth, while its poly-Q and ZZ domains act to restrain overgrowth. Further genetic and biochemical evidence indicates that orb2 functions upstream of the translational repressor Brain tumor (Brat), modulating Brat protein levels and, consequently, influencing brain size. These findings support a model wherein the antagonistic activities of Orb2 and Brat are critical for balanced brain growth during Drosophila neurodevelopment.
The CPEB ortholog Orb2 regulates brain size through the TRIM-NHL RNA-binding protein, Brain tumor.
CPEB 直系同源物 Orb2 通过 TRIM-NHL RNA 结合蛋白调节脑肿瘤的大小
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作者:Hailstock Taylor, Buehler Joseph, Robinson Beverly V, Low Timothy C H, Hua Yuqing, Adebambo Temitope H, Govaerts Jack, Schoborg Todd A, Lipshitz Howard D, Lerit Dorothy A
| 期刊: | bioRxiv | 影响因子: | 0.000 |
| 时间: | 2025 | 起止号: | 2025 Jul 22 |
| doi: | 10.1101/2025.07.18.665534 | 研究方向: | 肿瘤 |
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