PTEN mutations in autism spectrum disorder and congenital hydrocephalus: developmental pleiotropy and therapeutic targets

Tyrone DeSpenza,Marina Carlson,Shreyas Panchagnula,Stephanie M. Robert,Phan Q. Duy,Nell Mermin-Bunnell,Benjamin C. Reeves,Adam J. Kundishora,Aladine A. Elsamadicy,Hannah Smith,Jack Ocken,Seth L. Alper,Sheng Chih Jin,Ellen J. Hoffman,Kristopher T. Kahle

PTEN mutations in autism spectrum disorder and congenital hydrocephalus: developmental pleiotropy and therapeutic targets

2021

Tyrone DeSpenza
Marina Carlson
Shreyas Panchagnula
Stephanie M. Robert
Phan Q. Duy
Nell Mermin-Bunnell
Benjamin C. Reeves
Adam J. Kundishora
Aladine A. Elsamadicy
Hannah Smith
Jack Ocken
Seth L. Alper
Sheng Chih Jin
Ellen J. Hoffman
Kristopher T. Kahle

The lack of effective treatments for autism spectrum disorder (ASD) and congenital hydrocephalus (CH) reflects the limited understanding of the biology underlying these common neurodevelopmental disorders. Although ASD and CH have been extensively studied as independent entities, recent human genomic and preclinical animal studies have uncovered shared molecular pathophysiology. Here, we review and discuss phenotypic, genomic, and molecular similarities between ASD and CH, and identify the PTEN–PI3K–mTOR (phosphatase and tensin homolog–phosphoinositide 3-kinase–mammalian target of rapamycin) pathway as a common underlying mechanism that holds diagnostic, prognostic, and therapeutic promise for individuals with ASD and CH.

Keywords:

Phenotype
Tensin
pleiotropy
PTEN
Bioinformatics
Macrocephaly
Mechanism (biology)
Medicine
PI3K/AKT/mTOR pathway
Autism spectrum disorder

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