Differential roles of lysosomal cholesterol transporters in the development ofC. elegansNMJs

Author:

Guo Amin1,Wu Qi1,Yan Xin2,Chen Kanghua1,Liu Yuxiang1ORCID,Liang Dingfa3ORCID,Yang Yuxiao1,Luo Qunfeng1ORCID,Xiong Mingtao4,Yu Yong5ORCID,Fei Erkang4ORCID,Chen Fei1ORCID

Affiliation:

1. School of Basic Medical Sciences, Jiangxi Medical College, Nanchang University

2. School of Life Sciences, Nanchang University

3. Queen Mary School of Nanchang University

4. Institute of Biomedical Innovation, Jiangxi Medical College, Nanchang University

5. State Key Laboratory of Cellular Stress Biology, School of Life Sciences, Faculty of Medicine and Life Sciences, Xiamen University, Xiamen, China

Abstract

Cholesterol homeostasis in neurons is critical for synapse formation and maintenance. Neurons with impaired cholesterol uptake undergo progressive synapse loss and eventual degeneration. To investigate the molecular mechanisms of neuronal cholesterol homeostasis and its role during synapse development, we studied motor neurons ofCaenorhabditis elegansbecause these neurons rely on dietary cholesterol. Combining lipidomic analysis, we discovered that NCR-1, a lysosomal cholesterol transporter, promotes cholesterol absorption and synapse development. Loss ofncr-1causes smaller synapses, and low cholesterol exacerbates the deficits. Moreover, NCR-1 deficiency hinders the increase in synapses under high cholesterol. Unexpectedly, NCR-2, the NCR-1 homolog, increases the use of cholesterol and sphingomyelins and impedes synapse formation. NCR-2 deficiency causes an increase in synapses regardless of cholesterol concentration. Inhibiting the degradation or synthesis of sphingomyelins can induce or suppress the synaptic phenotypes inncr-2mutants. Our findings indicate that neuronal cholesterol homeostasis is differentially controlled by two lysosomal cholesterol transporters and highlight the importance of neuronal cholesterol homeostasis in synapse development.

Funder

MOST | National Natural Science Foundation of China

NIH Office of Research Infrastructure Programs

Publisher

Life Science Alliance, LLC

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