Author:
Cheung Stanley K. K.,Kwok Jacinda,Or Penelope M. Y.,Wong Chi Wai,Feng Bo,Choy Kwong Wai,Chang Raymond C. C.,Burbach J. Peter H.,Cheng Alfred S. L.,Chan Andrew M.
Abstract
AbstractPTEN hamartoma tumour syndrome is characterised by mutations in the human PTEN gene. We performed transcriptomic and proteomic analyses of neural tissues and primary cultures from heterozygous and homozygous Pten-knockout mice. The somatosensory cortex of heterozygous Pten-knockout mice was enriched in immune response and oligodendrocyte development Gene Ontology (GO) terms. Parallel proteomic analysis revealed differentially expressed proteins (DEPs) related to dendritic spine development, keratinisation and hamartoma signatures. However, primary astrocytes (ASTs) from heterozygous Pten-knockout mice were enriched in the extracellular matrix GO term, while primary cortical neurons (PCNs) were enriched in immediate-early genes. In ASTs from homozygous Pten-knockout mice, cilium-related activity was enriched, while PCNs exhibited downregulation of forebrain neuron generation and differentiation, implying an altered excitatory/inhibitory balance. By integrating DEPs with pre-filtered differentially expressed genes, we identified the enrichment of traits of intelligence, cognitive function and schizophrenia, while DEPs in ASTs were significantly associated with intelligence and depression.
Funder
Hong Kong Research Grants Council, Collaborative Research Fund
Brain and Mind Institute of the Chinese University of Hong Kong Pilot Project Fund
Lo Kwee-Seong Biomedical Research Seed Fund
Publisher
Springer Science and Business Media LLC
Cited by
2 articles.
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