Liver‐Derived Ketogenesis via Overexpressing HMGCS2 Promotes the Recovery of Spinal Cord Injury

Author:

Sun Xiaofei1,Zhang Bin1,Sun Kaiqiang1ORCID,Li Fudong1,Hu Dongping2,Chen Juxiang3,Kong Fanqi1,Xie Yang3

Affiliation:

1. Department of spine surgery, Changzheng Hospital Naval Medical University No.415 Fengyang Road Shanghai 200003 China

2. Shanghai Zechong Biotechnology Co., Ltd. Shanghai China

3. Department of Surgery, Changhai Hospital Naval Medical University No. 168 Changhai Road Shanghai 200433 China

Abstract

AbstractThe liver is the major ketogenic organ of the body, and ketones are reported to possess favorable neuroprotective effects. This study aims to elucidate whether ketone bodies generated from the liver play a critical role in bridging the liver and spinal cord. Mice model with a contusive spinal cord injury (SCI) surgery is established, and SCI induces significant histological changes in mice liver. mRNA‐seq of liver tissue shows the temporal changes of ketone bodies‐related genes, β‐hydroxybutyrate dehydrogenase (BDH1) and solute carrier family 16 (monocarboxylic acid transporters), member 6 (SLC16A6). Then, an activated ketogenesis model is created with adult C57BL/6 mice receiving the tail intravenous injection of GPAAV8‐TBG‐Mouse‐Hmgcs2‐CMV‐ mCherry ‐WPRE (HMGCS2liver) and mice receiving equal AAV8‐Null being the control group (Vectorliver). Then, the mice undergo either a contusive SCI or sham surgery. The results show that overexpression of HMG‐CoA synthase (Hmgcs2) in mice liver dramatically alleviates SCI‐mediated pathological changes and promotes ketogenesis in the liver. Amazingly, liver‐derived ketogenesis evidently alleviates neuron apoptosis and inflammatory microglia activation and improves the recovery of motor function of SCI mice. In conclusion, a liver‐spinal cord axis can be bridged via ketone bodies, and enhancing the production of the ketone body within the liver has neuroprotective effects on traumatic SCI.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

General Medicine

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