Abstract
GABAB receptors are heterodimeric G protein-coupled receptors, which control neuronal excitability by mediating prolonged inhibition. The magnitude of GABAB receptor-mediated inhibition essentially depends on the amount of receptors in the plasma membrane. However, the factors regulating cell surface expression of GABAB receptors are poorly characterized. Cell surface GABAB receptors are constitutively internalized and either recycled to the plasma membrane or degraded in lysosomes. The signal that sorts GABAB receptors to lysosomes is currently unknown. Here we show that Mind bomb-2 (MIB2)-mediated Lys-63-linked ubiquitination of the GABAB1 subunit at multiple sites is the lysosomal sorting signal for GABAB receptors. We found that inhibition of lysosomal activity in cultured rat cortical neurons increased the fraction of Lys-63-linked ubiquitinated GABAB receptors and enhanced the expression of total as well as cell surface GABAB receptors. Mutational inactivation of four putative ubiquitination sites in the GABAB1 subunit significantly diminished Lys-63-linked ubiquitination of GABAB receptors and prevented their lysosomal degradation. We identified MIB2 as the E3 ligase triggering Lys-63-linked ubiquitination and lysosomal degradation of GABAB receptors. Finally, we show that sustained activation of glutamate receptors, a condition occurring in brain ischemia that down-regulates GABAB receptors, considerably increased the expression of MIB2 and Lys-63-linked ubiquitination of GABAB receptors. Interfering with Lys-63-linked ubiquitination by overexpressing ubiquitin mutants or GABAB1 mutants deficient in Lys-63-linked ubiquitination prevented glutamate-induced down-regulation of the receptors. These findings indicate that Lys-63-linked ubiquitination of GABAB1 at multiple sites by MIB2 controls sorting of GABAB receptors to lysosomes for degradation under physiological and pathological conditions.
Highlights
An important factor regulating GABAB receptor signaling is the dynamic control of their cell surface expression via protein degradation
Inhibition of Lys-63-linked ubiquitination by overexpression of Ub(K63R) increased the expression level of cell surface GABAB receptors (GABAB1, 162 Ϯ 12%; GABAB2, 136 Ϯ 9% of control neurons transfected with wild-type ubiquitin; Fig. 2A), suggesting that GABAB receptor levels are regulated by Lys-63-linked ubiquitination
GABAB receptors assemble into heterodimeric GABAB1,2 complexes in the ER, which is a prerequisite for their ER exit and forward trafficking to the plasma membrane
Summary
An important factor regulating GABAB receptor signaling is the dynamic control of their cell surface expression via protein degradation. To test whether Lys-63-linked ubiquitination is involved in degrading GABAB receptors, we transfected neurons with a mutant of ubiquitin that is not able to form Lys-63linked chains (Ub(K63R)) and analyzed them for cell surface expression of GABAB receptors.
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