PQBP1

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Template:Short description Template:Infobox gene Polyglutamine-binding protein 1 (PQBP1) is a protein that in humans is encoded by the PQBP1 gene.[1][2][3]

Polyglutamine binding protein-1, which was identified as a binding protein to the polyglutamine tract sequence,[1][3] is an evolutionally conserved protein[4] expressed in various tissues including developmental[5] and adult brains[3] or mesodermal tissues.[6] In cells, PQBP1 is dominantly located in the nucleus[3][7] but also in the cytoplasm dependently on the cell type[8] and stress conditions.[9] PQBP1 has recently been found to play a role in the innate immune response of dendritic cells.[10]

It should be of note that PQBP1 has no relationship with QBP1, an artificial synthetic peptide.

Function

PQBP1 is a nuclear polyglutamine-binding protein that contains a WW domain.[3][11]

The molecular roles of PQBP1 are mainly in mRNA splicing[12][13] and transcription.[7][14] PQBP1 interacts with splicing proteins[15][16][17][18] and RNA-binding proteins.[19][20] PQBP1 deficiency critically affects mRNA splicing of cell cycle and synapse related genes.[12] Recent results indicated implication of PQBP1 in cytoplasmic RNA metabolism[21] and elongation of protein translation from mRNA.[22] Research also seems to suggest that PQBP1 also plays a role in the innate immune system as a necessary adaptor for the cGAS-mediated innate response to lentiviruses such as HIV1. This PQBP-1 dependent response initiates a sensor that detects lentiviral DNA.[23]

Clinical significance

Mutations in the PQBP1 gene, which encodes for this protein, have been known to cause X-linked intellectual disabilities (XLID), commonly referred to as Renpenning's syndrome.[24] Recent studies indicate that PQBP-1 interaction with TXNL4A is missing in patients with frameshift mutations causing Renpenning's syndrome. PQBP-1 seems to facilitate the nuclear import of TXNL4A, however the biological function of that interaction requires further investigation.[25] People who suffer from these disabilities share a common set of symptoms including: microcephaly, shortened stature and impaired intellectual development.[26] There are 11 types of mutations that have been identified, but the most common being frameshift mutations.[24][27] Other syndromic XLIDs such as Golabi-Ito-Hall syndrome and non-syndromic ID patients were also associated with PQBP1 gene mutations.[28][29][30]

Mutant Ataxin-1 and Huntingtin, disease proteins of spinocerebellar ataxia type-1 and Huntington's disease respectively, interact with PQBP1 and disturbed the functions of PQBP1.[7][31] Moreover, recent investigations revealed pathological roles of PQBP1 in neurons[32] and microglia[8] under neurodegeneration of Alzheimer's disease and tauopathy. SRRM2 phosphorylation detected in neurons at the early stage of Alzheimer's disease pathology[33] leads to reduction of SRRM2, a scaffold protein for RNA metabolism related molecules in the nucleus, which causes reduction of PQBP1 in the nucleus and acquired intellectual disability.[32] PQBP1 was shown as an intracellular receptor for HIV1 in dendritic cells[34] for innate immune system. Recent studies indicate that PQBP1 recognizes intact capsids of HIV-1 particles. It interacts with these capsids through its amino-terminus, and when capsid disassembles it triggers the PQBP-1 dependent recruitment of cGAS. This is crucial to activating the sensor that detects HIV-1 DNA as soon as synthesis is initiated.[23] Similarly, PQBP1 functions as an intracellular receptor for tau proteins and trigger brain inflammation.[8]

Animal models

Mouse models of knockdown and conditional knockout were generated, and they showed cognitive impairment and microcephaly.[35][12] The KD mice possess a transgene expressing 498 bp double-strand RNA that is endogenously cleaved to siRNA suppressing PQBP1 efficiently, and did not show obvious developmental abnormality.[35] Another knockdown model of the gene in mouse embryo primary neurons revealed a decrease in splicing efficiency and resulted in abnormal gastrulation and neuralation patterning.[6]

Drosophila models of underexpression and overexpression were also generated.[36][37] The hypomorph Drosophila model revealed molecular function of PQBP1 in learning acquisition mediated by decreased mRNA and protein expressions of NMDA receptor subunit NR1.[36] Research indicates that in order to appropriately function, the protein must be expressed within a critical range.[38][6]

References

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Further reading

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External links

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