Maintenance of the Neuroprotective Function of the Amino Group Blocked Fluorescence-Agmatine.
Sumit BaruaA Young SimJong Youl KimInjae ShinJong Eun LeePublished in: Neurochemical research (2021)
Agmatine, an endogenous derivative of arginine, has been found to be effective in treating idiopathic pain, convulsion, stress-mediated behavior, and attenuate the withdrawal symptoms of drugs like morphine. In the early stages of ischemic brain injury in animals, exogenous agmatine treatment was found to be neuroprotective. Agmatine is also considered as a putative neurotransmitter and is still an experimental drug. Chemically, agmatine is called agmatine 1-(4-aminobutyl guanidine). Crystallographic study data show that positively-charged guanidine can bind to the protein containing Gly and Asp residues, and the amino group can interact with the complimentary sites of Glu and Ser. In this study, we blocked the amino end of the agmatine by conjugating it with FITC, but the guanidine end was unchanged. We compared the neuroprotective function of the agmatine and agmatine-FITC by treating them in neurons after excitotoxic stimulation. We found that even the amino end blocked neuronal viability in the excitotoxic condition, by NMDA treatment for 1 h, was increased by agmatine-FITC, which was similar to that of agmatine. We also found that the agmatine-FITC treatment reduced the expression of nitric oxide production in NMDA-treated cells. This study suggests that even if the amino end of agmatine is blocked, it can perform its neuroprotective function.
Keyphrases
- brain injury
- nitric oxide
- cerebral ischemia
- subarachnoid hemorrhage
- emergency department
- machine learning
- poor prognosis
- small molecule
- electronic health record
- combination therapy
- spinal cord injury
- cell death
- signaling pathway
- induced apoptosis
- pain management
- heat stress
- replacement therapy
- amino acid
- cell cycle arrest