Neuronal SEL1L-HRD1 ER-associated degradation is essential for motor function and survival in mice
Mauricio Torres, You Lu, Brent Pederson, Hui Wang, Anna Gretzinger, Liangguang Lin, Jiwon Hwang, Xinxin Chen, Alan C. Rupp, Abigail J. Tomlinson, Andrew J. Scott, Zhen Zhao, Daniel R. Wahl, Martin Myers, Jr, Costas A. Lyssiotis, Ling Qi
Mauricio Torres, You Lu, Brent Pederson, Hui Wang, Anna Gretzinger, Liangguang Lin, Jiwon Hwang, Xinxin Chen, Alan C. Rupp, Abigail J. Tomlinson, Andrew J. Scott, Zhen Zhao, Daniel R. Wahl, Martin Myers, Jr, Costas A. Lyssiotis, Ling Qi
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Neuronal SEL1L-HRD1 ER-associated degradation is essential for motor function and survival in mice

Abstract

Hypomorphic variants in the SEL1L-HRD1 ER-associated degradation (ERAD) complex have been linked to severe neurological syndromes in children, including neurodevelopmental delay, intellectual disability, motor dysfunction, and early death. Despite this association, its physiological importance and underlying mechanisms in neurons remain poorly understood. Here, we show that neuronal SEL1L-HRD1 ERAD is essential for maintaining one-carbon metabolism, motor function, and overall viability. Neuron-specific deletion of Sel1L in mice (Sel1LSynCre) resulted in growth retardation, severe motor impairments, and early mortality by 9 weeks of age—mirroring core clinical features observed in affected patients—despite preserved neuronal numbers and only modest ER stress. Multi-omics analyses, including single-nucleus RNA sequencing and metabolomics, revealed significant dysregulation of one-carbon metabolism in ERAD-deficient brains. This included activation of the serine, folate, and methionine pathways, accompanied by elevated levels of S-adenosylmethionine and related metabolites, likely resulted from induction of the integrated stress response (ISR). Together, these findings uncover a previously unappreciated role for neuronal SEL1L-HRD1 ERAD in coordinating ER protein quality control with metabolic adaptation, providing new insight into the molecular basis of ERAD-related neurodevelopmental disease.

Authors

Mauricio Torres, You Lu, Brent Pederson, Hui Wang, Anna Gretzinger, Liangguang Lin, Jiwon Hwang, Xinxin Chen, Alan C. Rupp, Abigail J. Tomlinson, Andrew J. Scott, Zhen Zhao, Daniel R. Wahl, Martin Myers, Jr, Costas A. Lyssiotis, Ling Qi

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Supplemental video 2: Hindlimb clasping reflex in Sel1Lf/f and Sel1LSynCre mice at 2 weeks of age. The hindlimb clasping reflex was assessed via tail suspension in control (Sel1Lf/f) and neuron-specific Sel1L knockout (Sel1LSynCre) mice at postnatal day 14. Healthy mice typically extend their hindlimbs outward when suspended by the tail. In contrast, Sel1LSynCre mice exhibit an abnormal clasping phenotype, retracting their hindlimbs toward the midline of the body. - Download (4.63 MB)

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