Exosomes are secreted membrane vesicles that share structural and biochemical characteristics with intraluminal vesicles of multivesicular endosomes (MVEs). Exosomes could be involved in intercellular communication and in the pathogenesis of infectious and degenerative diseases. The molecular mechanisms of exosome biogenesis and secretion are, however, poorly understood. Using a RNA interference screen, we identified five RabGTPases that promote exosome secretion in HeLa cells. Among these, Rab27a and Rab27b were found to act in MVE docking at the plasma membrane. The size of MVEs was strongly increased by Rab27a silencing, whereas MVEs were redistributed towards the perinuclear region upon Rab27b silencing. Thus, the two Rab27 isoforms play different roles in the exosomal pathway. In addition, silencing two known Rab27 effectors, Slp4 (SYTL4) and Slac2b (EXPH5), inhibited exosome secretion and phenocopied silencing of Rab27a and Rab27b, respectively. Our results therefore strengthen the link between MVEs and exosomes, and open ways to manipulate exosome secretion in vivo.3
Innate immune cells detect pathogens via pattern recognition receptors (PRRs), which signal for initiation of immune responses to infection. Studies with Dectin-1, a PRR for fungi, have defined a novel innate signaling pathway involving Syk kinase and the adaptor CARD9, which is critical for inducing Th17 responses to fungal infection. We show that another C-type lectin, Dectin-2, also signals via Syk and CARD9, and contributes to dendritic cell (DC) activation by fungal particles. Unlike Dectin-1, Dectin-2 couples to Syk indirectly, through association with the FcRγ chain. In a model of Candida albicans infection, blockade of Dectin-2 did not affect innate immune resistance but abrogated Candida-specific T cell production of IL-17 and, in combination with the absence of Dectin-1, decreased Th1 responses to the organism. Thus, Dectin-2 constitutes a major fungal PRR that can couple to the Syk–CARD9 innate signaling pathway to activate DCs and regulate adaptive immune responses to fungal infection.
The transition from naïve to activated T cells is marked by alternative splicing of pre-mRNA encoding the transmembrane phosphatase CD45. Using a short hairpin RNA interference screen, we identified heterogeneous ribonucleoprotein L-like (hnRNPLL) as a critical inducible regulator of CD45 alternative splicing. HnRNPLL was up-regulated in stimulated T cells, bound CD45 transcripts, and was both necessary and sufficient for CD45 alternative splicing. Depletion or overexpression of hnRNPLL in B and T cell lines and primary T cells resulted in reciprocal alteration of CD45RA and RO expression. Exon array analysis suggested that hnRNPLL acts as a global regulator of alternative splicing in activated T cells. Induction of hnRNPLL during hematopoietic cell activation and differentiation may allow cells to rapidly shift their transcriptomes to favor proliferation and inhibit cell death.It is estimated that greater than 75% of genes yield alternative transcripts, contributing to considerable functional diversity within the genome (1,2). SR (serine-arginine rich) proteins are key positive regulators of alternative splicing that bind enhancer sequences on nascent transcripts and recruit spliceosomal proteins to weak splice sites, thereby facilitating proximal spliceo-some assembly (3). Heterogeneous nuclear ribonucleoproteins (hnRNPs) also regulate splicing by binding negative cis-regulatory elements and causing exon exclusion from mature mRNA (3). SR proteins and hnRNPs function as antagonists in alternative splicing, with binding of hnRNPs to silencer sequences inhibiting SR protein binding, thus forcing a shift of splicing to distal splice sites (4).CD45 is an abundant transmembrane protein tyrosine phosphatase expressed at the surface of T cells, B cells, and other hematopoietic cells (5). CD45 transcripts undergo extensive alternative splicing in which exons 4, 5, and 6 are variably excluded (Fig. 1A) (6). Primary naive T cells and B cells express the larger isoforms and are referred to as RA + . In contrast, activated and memory T cells express the shortest isoform, CD45RO (5). CD45 initiates signaling through antigen receptors by dephosphorylating the inhibitory tyrosine on Src-family kinases (5), but attributing specific functions to individual CD45
Innate immune cells detect pathogens via pattern recognition receptors (PRRs),
HIV-1 is a complex retrovirus that uses host machinery to promote its replication. Understanding cellular proteins involved in the multistep process of HIV-1 infection may result in the discovery of more adapted and effective therapeutic targets. Kinases and phosphatases are a druggable class of proteins critically involved in regulation of signal pathways of eukaryotic cells. Here, we focused on the discovery of kinases and phosphatases that are essential for HIV-1 replication but dispensable for cell viability. We performed an iterative screen in Jurkat T-cells with a short-hairpin-RNA (shRNA) library highly enriched for human kinases and phosphatases. We identified 14 new proteins essential for HIV-1 replication that do not affect cell viability. These proteins are described to be involved in MAPK, JNK and ERK pathways, vesicular traffic and DNA repair. Moreover, we show that the proteins under study are important in an early step of HIV-1 infection before viral integration, whereas some of them affect viral transcription/translation. This study brings new insights for the complex interplay of HIV-1/host cell and opens new possibilities for antiviral strategies.
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