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  • Reversal of autism-like behaviors and metabolism in adult mice with single-dose antipurinergic therapy.

Reversal of autism-like behaviors and metabolism in adult mice with single-dose antipurinergic therapy.

Translational psychiatry (2014-06-18)
J C Naviaux, M A Schuchbauer, K Li, L Wang, V B Risbrough, S B Powell, R K Naviaux
초록

Autism spectrum disorders (ASDs) now affect 1-2% of the children born in the United States. Hundreds of genetic, metabolic and environmental factors are known to increase the risk of ASD. Similar factors are known to influence the risk of schizophrenia and bipolar disorder; however, a unifying mechanistic explanation has remained elusive. Here we used the maternal immune activation (MIA) mouse model of neurodevelopmental and neuropsychiatric disorders to study the effects of a single dose of the antipurinergic drug suramin on the behavior and metabolism of adult animals. We found that disturbances in social behavior, novelty preference and metabolism are not permanent but are treatable with antipurinergic therapy (APT) in this model of ASD and schizophrenia. A single dose of suramin (20 mg kg(-1) intraperitoneally (i.p.)) given to 6-month-old adults restored normal social behavior, novelty preference and metabolism. Comprehensive metabolomic analysis identified purine metabolism as the key regulatory pathway. Correction of purine metabolism normalized 17 of 18 metabolic pathways that were disturbed in the MIA model. Two days after treatment, the suramin concentration in the plasma and brainstem was 7.64 μM pmol μl(-1) (±0.50) and 5.15 pmol mg(-1) (±0.49), respectively. These data show good uptake of suramin into the central nervous system at the level of the brainstem. Most of the improvements associated with APT were lost after 5 weeks of drug washout, consistent with the 1-week plasma half-life of suramin in mice. Our results show that purine metabolism is a master regulator of behavior and metabolism in the MIA model, and that single-dose APT with suramin acutely reverses these abnormalities, even in adults.

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Sigma-Aldrich
Polyinosinic–polycytidylic acid potassium salt, with buffer salts, TLR ligand tested
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Potassium hydride, in paraffin
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Potassium, chunks (in mineral oil), 98% trace metals basis
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Formic acid, ≥95%, FCC, FG
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Formic acid solution, BioUltra, 1.0 M in H2O
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Potassium hydride, 30 wt % dispersion in mineral oil
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Ammonium hydroxide solution, BioUltra, ~1 M NH3 in H2O (T)
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Ammonium hydroxide solution, puriss. p.a. plus, ≥25% NH3 in H2O
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Formic acid, ACS reagent, ≥96%
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Ammonium hydroxide solution, puriss., meets analytical specification of Ph. Eur., 25-30% NH3 basis
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Ammonium hydroxide solution, puriss., 30-33% NH3 in H2O
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Formic acid, ACS reagent, ≥88%
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Formic acid, puriss., meets analytical specifications of DAC, FCC, 98.0-100%
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Ammonium hydroxide solution, ACS reagent, 28.0-30.0% NH3 basis
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Ammonium hydroxide solution, puriss. p.a., reag. ISO, reag. Ph. Eur., ~25% NH3 basis
Sigma-Aldrich
Formic acid, reagent grade, ≥95%
Sigma-Aldrich
Formic acid, puriss. p.a., ACS reagent, reag. Ph. Eur., ≥98%
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Ammonium hydroxide solution, 28% NH3 in H2O, ≥99.99% trace metals basis