Social memory, amnesia, and autism: brain oxytocin secretion is regulated by NAD+ metabolites and single nucleotide polymorphisms of CD38

Haruhiro Higashida; Shigeru Yokoyama; Jian-Jun Huang; Li Liu; Wen-Jie Ma; Shirin Akther; Chiharu Higashida; Mitsuru Kikuchi; Yoshio Minabe; Toshio Munesue

doi:10.1016/j.neuint.2012.01.030

Social memory, amnesia, and autism: brain oxytocin secretion is regulated by NAD+ metabolites and single nucleotide polymorphisms of CD38

Neurochem Int. 2012 Nov;61(6):828-38. doi: 10.1016/j.neuint.2012.01.030. Epub 2012 Feb 13.

Authors

Haruhiro Higashida¹, Shigeru Yokoyama, Jian-Jun Huang, Li Liu, Wen-Jie Ma, Shirin Akther, Chiharu Higashida, Mitsuru Kikuchi, Yoshio Minabe, Toshio Munesue

Affiliation

¹ Department of Biophysical Genetics, Kanazawa University Graduate School of Medicine, Kanazawa 920-8640, Japan. haruhiro@med.kanazawa-u.ac.jp

PMID: 22366648
DOI: 10.1016/j.neuint.2012.01.030

Abstract

Previously, we demonstrated that CD38, a transmembrane protein with ADP-ribosyl cyclase activity, plays a critical role in mouse social behavior by regulating the release of oxytocin (OXT), which is essential for mutual recognition. When CD38 was disrupted, social amnesia was observed in Cd38 knockout mice. The autism spectrum disorders (ASDs), characterized by defects in reciprocal social interaction and communication, occur either sporadically or in a familial pattern. However, the etiology of ASDs remains largely unknown. Therefore, the theoretical basis for pharmacological treatments has not been established. Hence, there is a rationale for investigating single nucleotide polymorphisms (SNPs) in the human CD38 gene in ASD subjects. We found several SNPs in this gene. The SNP rs3796863 (C>A) was associated with high-functioning autism (HFA) in American samples from the Autism Gene Resource Exchange. Although this finding was partially confirmed in low-functioning autism subjects in Israel, it has not been replicated in Japanese HFA subjects. The second SNP of interest, rs1800561 (4693C>T), leads to the substitution of an arginine (R) at codon 140 by tryptophan (W; R140W) in CD38. This mutation was found in four probands of ASD and in family members of three pedigrees with variable levels of ASD or ASD traits. The plasma levels of OXT in ASD subjects with the R140W allele were lower than those in ASD subjects lacking this allele. The OXT levels were unchanged in healthy subjects with or without this mutation. One proband with the R140W allele receiving intranasal OXT for approximately 3years showed improvement in areas of social approach, eye contact and communication behaviors, emotion, irritability, and aggression. Five other ASD subjects with mental deficits received nasal OXT for various periods; three subjects showed improved symptoms, while two showed little or no effect. These results suggest that SNPs in CD38 may be possible risk factors for ASD by abrogating OXT function and that some ASD subjects can be treated with OXT in preliminary clinical trials.

MeSH terms

ADP-ribosyl Cyclase / metabolism
ADP-ribosyl Cyclase 1 / genetics
ADP-ribosyl Cyclase 1 / immunology*
Administration, Intranasal
Amnesia / genetics
Amnesia / metabolism
Amnesia / physiopathology*
Animals
Autistic Disorder / genetics
Autistic Disorder / metabolism
Autistic Disorder / physiopathology*
Brain / metabolism*
Exons
Humans
Introns
Memory*
Mice
Mice, Knockout
NAD / metabolism*
Oxytocin / administration & dosage
Oxytocin / metabolism*
Polymorphism, Single Nucleotide*
Vasopressins / metabolism

Substances

NAD
Vasopressins
Oxytocin
ADP-ribosyl Cyclase
ADP-ribosyl Cyclase 1