Recombinant Mouse Protein phosphatase 1 regulatory subunit 1B (Ppp1r1b)

1. This study strongly suggests that inflammation-regulated DARPP-32 constitutes a key component of H. pylori-mediated gastric tumourigenesis. PMID: 27590997
2. the results suggest that by inducing dephosphorylation of DARPP-32 at Ser-97 and altering its cytonuclear distribution, glutamate may counteract dopamine/D1 receptor/PKA signaling at multiple cellular levels. PMID: 27998980
3. Darpp32 interaction with beta-adducin may be the molecular pathway by which environmental changes may rapidly alter responsiveness of striatal neurons involved in the reward system. PMID: 26639316
4. Results show that Darpp-32 was expressed in normal mouse mammary tissue and in some breast tumors, whereas t-Darpp was found exclusively in mammry tumors. PMID: 25128420
5. analysis of cAMP-activated DARPP-32 signalling to the nucleus PMID: 25692798
6. Results describe the development of new vascular mouse model with a conditional knockout allele of Tsc1 with a Darpp32-Cre allele. This mouse displayed accelerated formation of both kidney cystadenomas and paw hemangiosarcomas. PMID: 25548102
7. Cannabinoid-stimulated G-protein activity did not differ between DARPP-32 KO and WT mice treated with vehicle or repeated THC. PMID: 26099530
8. In this work, the dissected postsynaptic topology of the DARPP-32 phosphoprotein provides strong evidence for a compartmentalized and confined distribution in dendritic spines. PMID: 24058659
9. Adenosine AA receptors in striatal glutamatergic terminals and GABAergic neurons oppositely modulate psychostimulant action and DARPP-32 phosphorylation. PMID: 24312250
10. This study demonistrated that environment enhanced Darpp32 expression in brain and enhanced totaroad perfermance and short term working menory. PMID: 23558143
11. DARPP32 has a role in pluripotent stem cell differentiation toward medium-sized spiny neurons PMID: 23250204
12. l-DOPA-induced activation of ERK and mTORC1 requires DARPP-32 and indicates the importance of the cAMP/DARPP-32 signaling cascade in dyskinesia. PMID: 22753408
13. DARPP-32 increases interactions between epidermal growth factor receptor and ERBB3 to promote tumor resistance to gefitinib. PMID: 21741919
14. Data show that the loss of DARPP-32 in striatopallidal neurons produced a robust increase in locomotor activity. PMID: 20682746
15. results indicate that under chronic dopamine deficiency (a) the A(2A)/cAMP/PKA/DARPP-32 cascade is overactive due to the elevated endogenous phospho-DARPP-32 levels and (b) the A(2A) receptor modulatory effect on ERK1/2 signaling is dysregulated PMID: 19852993
16. Our data demonstrate that beta(1)- and alpha(2)-adrenoceptors regulate DARPP-32 phosphorylation in neostriatal neurons. PMID: 20236221
17. Data confirmed that CR specifically increased dopamine- and cAMP-regulated phosphoprotein (Darpp-32), a key regulator of dopamine receptor signaling, in the amygdala. PMID: 19737990
18. DARPP-32 is essential not only for dopaminergic but also for serotonergic neurotransmission. PMID: 11880652
19. stimulatory effect of caffeine on motor activity in mice was greatly reduced following genetic deletion of DARPP-32 (dopamine- and cyclic AMP-regulated phosphoprotein of relative molecular mass 32,000) PMID: 12181566
20. adenosine A(2A)DARPP-32 signaling is stimulated by mGlu receptors by stimulating the adenosine A(2A) receptor-mediated formation of cAMP in an extracellular signal-regulated kinase-dependent manner PMID: 12538871
21. data demonstrate that the effects of psychotomimetics on sensorimotor gating and repetitive movements depend on DARPP-32; they regulate, through distinct mechanisms, phosphorylation of DARPP-32 as well as downstream effectors in the cortex and striatum PMID: 14631045
22. Blockade of the ERK pathway or mutation of DARPP-32 altered locomotor sensitization induced by a single injection of psychostimulants, demonstrating the functional relevance of this regulation. PMID: 15608059
23. These data indicate a potential role for DARPP-32 and inhibitor-1 in the regulation of PP1 activity in pancreatic beta-cell stimulus-secretion coupling. PMID: 15737638
24. these findings highlight distinct roles of the Thr-34 and Thr-75 phosphorylation sites of DARPP-32 in mediating short- and long-term behavioral and biochemical actions of cocaine PMID: 16123776
25. Psychomotor effect of cannabinoids can be accounted for by striatal projection neurons involving protein kinase A-dependent phosphorylation of DARPP-32. PMID: 16162925
26. DARPP-32 plays a key role for development of D1R motor stimulatory effects in mice PMID: 16189209
27. The results indicate that DARPP-32 is involved in the retinal pathway transmitting photic information that resets the circadian clock. PMID: 16971527
28. multiple signal transduction pathways mediating expression of DARPP-32 in vitro, including a novel, important pathway via by which PI3K regulates the contribution of cdk5/p35. PMID: 17209049
29. These data indicate that DARPP-32 participates in dopamine-mediated modifications of retinal function. PMID: 17552992
30. The abnormal involuntary movements developed in response to chronic L-DOPA are due to hyperactivation in striatal medium spiny neurons of a signaling pathway including sequential phosphorylation of DARPP-32, ERK1/2, MSK-1, and histone H3. PMID: 17596448
31. although DARPP-32 impacts cortical inhibition through a previously demonstrated D2-dependent regulation of GABAergic currents in pyramidal cells, it is not involved in the direct D1-mediated regulation of fast-spiking interneurons PMID: 17693396
32. DARPP-32 plays a central role in 1) modulating intercellular coupling, 2) cortical excitatory drive of spiny and aspiny GABAergic neurons, and 3) local feedforward inhibitory drive of cholinergic-like interneurons within accumbens circuits. PMID: 18155847
33. The nuclear accumulation of DARPP-32, a potent inhibitor of protein phosphatase-1, increases the phosphorylation of histone H3, an important component of nucleosomal response. PMID: 18496528
34. Csnk1-epsilon is crucial for the locomotor stimulant response to a moderate dose of MA and suggest that genetic polymorphisms affecting Csnk1-epsilon expression or function could influence sensitivity to amphetamines in both mice and humans. PMID: 19050854

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KEGG: mmu:19049

STRING: 10090.ENSMUSP00000077760

UniGene: Mm.45372