MBP-activated autoimmunity plays a role in arsenic-induced peripheral neuropathy and the potential protective effect of mecobalamin.
Qican HeBingzhi ChenShaoyi ChenMuyang ZhangLidan DuanXiangling FengJihua ChenLezhou ZhouLv ChenYanying DuanPublished in: Environmental toxicology (2021)
Intake excessive arsenic (As) is related to the occurrence of peripheral neuropathy. However, both the underlying mechanism and the preventive approach remain largely unknown. In the present study, As treatment significantly decreased the mechanical withdrawal threshold and increased the titer of anti-myelin basic protein antibody in rats, accompanied with damaged BNB. The levels of inflammatory cytokines and proteolytic enzymes were also significantly upregulated. However, administration of MeCbl in As-treated rats significantly reversed the decline in hindfoot mechanical withdrawal threshold, as well as BNB failure and sciatic nerve inflammation. Repeated As treatment in athymic nude mice indicated that sciatic nerve inflammation and mechanical hyperalgesia were T cell-dependent. These data implicated that MBP-activated autoimmunity and the related neuroinflammation probably contributed to As-induced mechanical hyperalgesia and MeCbl exerted a protective role probably via maintenance the integrity of BNB and inhibition of neuroinflammation.
Keyphrases
- oxidative stress
- diabetic rats
- high glucose
- traumatic brain injury
- drinking water
- risk assessment
- drug induced
- lipopolysaccharide induced
- neuropathic pain
- big data
- cognitive impairment
- adipose tissue
- multiple sclerosis
- small molecule
- skeletal muscle
- combination therapy
- protein protein
- artificial intelligence
- metabolic syndrome
- blood brain barrier
- inflammatory response
- deep learning
- climate change
- spinal cord