Proc Natl Acad Sci U S A. 2011 Nov 15;108(46):18831-6. Epub 2011 Nov 2.

Schizophrenia susceptibility gene dysbindin regulates glutamatergic and dopaminergic functions via distinctive mechanisms in Drosophila.

Shao L, Shuai Y, Wang J, Feng S, Lu B, Li Z, Zhao Y, Wang L, Zhong Y.

Source

School of Life Sciences, Tsinghua University, Beijing 100084, People's Republic of China.

Abstract

The dysfunction of multiple neurotransmitter systems is a striking pathophysiological feature of many mental disorders, schizophrenia in particular, but delineating the underlying mechanisms has been challenging. Here we show that manipulation of a single schizophrenia susceptibility gene, dysbindin, is capable of regulating both glutamatergic and dopaminergic functions through two independent mechanisms, consequently leading to two categories of clinically relevant behavioral phenotypes. Dysbindin has been reported to affect glutamatergic and dopaminergic functions as well as a range of clinically relevant behaviors in vertebrates and invertebrates but has been thought to have a mainly neuronal origin. We find that reduced expression of Drosophila dysbindin (Ddysb) in presynaptic neurons significantly suppresses glutamatergic synaptic transmission and that this glutamatergic defect is responsible for impaired memory. However, only the reduced expression of Ddysb in glial cells is the cause of hyperdopaminergic activities that lead to abnormal locomotion and altered mating orientation. This effect is attributable to the altered expression of a dopamine metabolic enzyme, Ebony, in glial cells. Thus, Ddysb regulates glutamatergic transmission through its neuronal function and regulates dopamine metabolism by regulating Ebony expression in glial cells.

PMID:: 22049342; [PubMed - indexed for MEDLINE]
PMCID:: PMC3219129

Free PMC Article

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Fig. 2.

Tissue-specific regulation of changes in different neurotransmitter systems and behaviors. (A) EJC amplitude was reduced significantly by expression of the Ddysb RNAi presynaptically (elav-Gal4/Y; DdysbIR-1/⁺) but not postsynaptically (DdysbIR-1/⁺;C57/⁺) (ANOVA; n = 9–16). The calcium concentration for recording is 0.4 mM. (B) Neuronal expression of UAS-Ddysb (elav-Gal4/Y;UAS-Ddysb/⁺;dysb¹) rescued the EJC deficit in the dysb¹ mutant (ANOVA; n = 16–22). (C) Glial expression of Ddysb (UAS-Ddysb/⁺;Repo-Gal4 dysb¹/dysb¹), but not neuronal expression of Ddysb (UAS-Ddysb/⁺;elav-Gal4_(III) dysb¹/dysb¹), restored the brain dopamine concentration to normal levels (ANOVA; n = 5–10). (D) Pan-neural expression of Ddysb (UAS-Ddysb/⁺;elav-Gal4_(III) dysb¹/dysb¹) is sufficient to rescue the 3-min associative memory deficit in the dysb¹ mutant. However, glia-specific expression of Ddysb (UAS-Ddysb/⁺;Repo-Gal4 dysb¹/dysb¹) failed to do so (ANOVA; n = 4–14). (E and F) Locomotor hyperactivity and mating disorientation were suppressed in dysb¹ mutants expressing UAS-Ddysb in glia (UAS-Ddysb/⁺;Repo-Gal4 dysb¹/dysb¹) but not in neurons (UAS-Ddysb/⁺;elav-Gal4_(III) dysb¹/dysb¹). (ANOVA; n = 8–10 for locomotor test; n = 22–51 for mating test.) Data are means ± SEM. (G and I) Pan-neuronal expression of Hdysb rescued the EJC amplitude (elav-Gal4/Y;UAS-Hdysb/⁺;dysb¹) (ANOVA; n = 9–10) and the 3-min associative memory deficit (UAS-Hdysb/⁺;elav-Gal4_(III) dysb¹/dysb¹) (ANOVA; n = 16) in the dysb¹ mutant. Calcium concentration for recording is 0.4 mM. (H and J) Glial expression of Hdysb (UAS-Hdysb/⁺;Repo-Gal4 dysb¹/dysb¹) restored the brain dopamine level (ANOVA; n = 4–11) and partially suppressed the hyperactivity in the dysb¹ mutant (ANOVA; n = 10). Data are means ± SEM. *P < 0.05; **P < 0.01; ***P < 0.001; n.s., not significant (P > 0.05).

Schizophrenia susceptibility gene dysbindin regulates glutamatergic and dopaminergic functions via distinctive mechanisms in Drosophila

Proc Natl Acad Sci U S A. Proc Natl Acad Sci U S A;108(46):18831-18836.