P2X4 receptors in activated C8-B4 cells of cerebellar microglial origin

Toulmé, Estelle; Garcia, Angie; Samways, Damien S. K.; Egan, Terrance M.; Khakh, Baljit S.

doi:10.1083/jcb1892oia7

Cited by 5 publications

(9 citation statements)

References 61 publications

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“…However, despite numerous attempts, P2X4R‐evoked currents could not be detected in microglia 48h after induction of SE. Activity of P2X4R is tightly regulated by a balance between rapid, activity‐dependent endocytosis, and membrane insertion of the protein (Qureshi et al, ; Toulme et al, ). The large amount of ATP released during slice processing is likely to promote the rapid endocytosis of P2X4R, precluding the recording of its activity in acute brain slices.…”

Section: Discussionmentioning

confidence: 99%

Involvement of P2X4 receptors in hippocampal microglial activation afterstatus epilepticus

Ulmann¹,

Levavasseur²,

Avignone³

et al. 2013

Glia

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Within the central nervous system, functions of the ATP-gated receptor-channel P2X4 (P2X4R) are still poorly understood, yet P2X4R activation in neurons and microglia coincides with high or pathological neuronal activities. In this study, we investigated the potential involvement of P2X4R in microglial functions in a model of kainate (KA)-induced status epilepticus (SE). We found that SE was associated with an induction of P2X4R expression in the hippocampus, mostly localized in activated microglial cells. In P2X4R-deficient mice, behavioral responses during KA-induced SE were unaltered. However, 48h post SE specific features of microglial activation, such as cell recruitment and upregulation of voltage-dependent potassium channels were impaired in P2X4R-deficient mice, whereas the expression and function of other microglial purinergic receptors remained unaffected. Consistent with the role of P2X4R in activity-dependent degenerative processes, the CA1 area was partially protected from SE-induced neuronal death in P2X4R-deficient mice compared with wild-type animals. Our findings demonstrate that P2X4Rs are brought into play during neuronal hyperexcitability and that they control specific aspects of microglial activation. Our results also suggest that P2X4Rs contribute to excitotoxic damages by regulating microglial activation.

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Section: Discussionmentioning

confidence: 99%

Involvement of P2X4 receptors in hippocampal microglial activation afterstatus epilepticus

Ulmann¹,

Levavasseur²,

Avignone³

et al. 2013

Glia

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“…For reverse transcriptase (RT)-polymerase chain reaction (PCR), first strand cDNA was synthesized (Amersham Biosciences, NJ) and amplified by PCR using specific primers as described (Ploix et al 2001; Schmid et al 2009). Real-time PCR was performed using the iQ5 real-time PCR detection system (Bio-Rad) and primer sequences described in (Noor et al 2010; Toulme et al 2010). The relative number of CCL21 transcripts per hypoxanthine phosphoribosyl transferase (HPRT) transcripts was determined by using calibration standards for both HPRT and CCL21 as previously described (Toulme et al 2010).…”

Section: Methodsmentioning

confidence: 99%

“…Real-time PCR was performed using the iQ5 real-time PCR detection system (Bio-Rad) and primer sequences described in (Noor et al 2010; Toulme et al 2010). The relative number of CCL21 transcripts per hypoxanthine phosphoribosyl transferase (HPRT) transcripts was determined by using calibration standards for both HPRT and CCL21 as previously described (Toulme et al 2010). Briefly, PCR fragments served as standards for calibration of quantitative PCR were purified from preparative gels with an extraction kit (QiAquick; Qiagen Germany).…”

Section: Methodsmentioning

confidence: 99%

CNS-derived CCL21 is both sufficient to drive homeostatic CD4+ T cell proliferation and necessary for efficient CD4+ T cell migration into the CNS parenchyma following Toxoplasma gondii infection

Ploix¹,

Noor²,

Crane³

et al. 2011

Brain, Behavior, and Immunity

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Injury, infection and autoimmune triggers increase CNS expression of the chemokine CCL21. Outside the CNS, CCL21 contributes to chronic inflammatory disease and autoimmunity by three mechanisms: recruitment of lymphocytes into injured or infected tissues, organization of inflammatory infiltrates into lymphoid-like structures and promotion of homeostatic CD4+ T-cell proliferation. To test if CCL21 plays the same role in CNS inflammation, we generated transgenic mice with astrocyte-driven expression of CCL21 (GFAP-CCL21 mice). Astrocyte-produced CCL21 was bioavailable and sufficient to support homeostatic CD4+ T-cell proliferation in cervical lymph nodes even in the absence of endogenous CCL19/CCL21. However, lymphocytes and glial-activation were not detected in the brains of uninfected GFAP-CCL21 mice, although CCL21 levels in GFAP-CCL21 brains were higher than levels expressed in inflamed Toxoplasmainfected nontransgenic brains. Following Toxoplasma infection, T-cell extravasation into submeningeal, perivascular and ventricular sites of infected CNS was not CCL21-dependent, occurring even in CCL19/CCL21-deficient mice. However, migration of extravasated CD4+, but not CD8+ T cells from extra-parenchymal CNS sites into the CNS parenchyma was CCL21-dependent. CD4+ T cells preferentially accumulated at perivascular, submeningeal and ventricular spaces in infected CCL21/CCL19-deficient mice. By contrast, greater numbers of CD4+ T cells infiltrated the parenchyma of infected GFAP-CCL21 mice than in wild-type or CCL19/CCL21-deficient mice. Together these data indicate that CCL21 expression within the CNS has the potential to contribute to T cell-mediated CNS pathology via: (a) homeostatic priming of CD4+ Tlymphocytes outside the CNS and (b) by facilitating CD4+ T-cell migration into parenchymal sites following pathogenic insults to the CNS.

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“…However, in a subsequent study, amitriptyline was found to have no effect at recombinant human P2X4 receptors and to act as a noncompetitive antagonist at recombinant rat and mouse P2X4 receptors 59. Interestingly, one group did find an inhibitory effect of tricyclic antidepressants and serotonin uptake inhibitors on native P2X4 receptors in mouse cerebellar microglia,60 but they concluded that this was due to inhibition of trafficking of the P2X4 receptors to the plasma membrane, rather than antagonism of the receptor per se .…”

Section: P2x4 Receptorsmentioning

confidence: 96%

Pharmacology of P2X receptors

Syed

Kennedy

2011

WIREs Membr Transp Signal

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P2X receptors are ligand-gated cation channels that mediate many of the extracellular actions of adenosine 5 -triphosphate (ATP). The genes encoding seven different P2X subunits, P2X1-7, have been cloned and when expressed alone all P2X subunits form functional receptors, except P2X6, which usually only assembles in a heteromeric form. Subunits can also interact with each other and to date seven functional heteromultimers with pharmacological and/or biophysical properties that differ from the individual homomultimers have been identified: P2X2/3, P2X4/6, P2X1/5, P2X2/6, P2X1/4, P2X1/2, and possibly P2X4/7. These are distributed widely throughout the body and are involved in many physiological and pathophysiological processes. ATP is an agonist at all subtypes and few selective agonists and no useful antagonists were available when P2X receptors were first defined. Subsequently, nonselective antagonists, such as suramin and PPADS, were discovered and since then, and particularly in the past decade, numerous potent and subtype-selective antagonists have been developed. These include NF449 and RO-1 at P2X1 receptors; PSB-1011 at P2X2 receptors; A317491, compound A, RO-3, and AF-353 at P2X3 and P2X2/3 receptors; 5-BDBD at P2X4 receptors; and A740003, A438079, A804598, GSK314181A, AZ10606120, AZ11645373, AZD-9056, CE-224535, and EVT-401 at P2X7 receptors. The therapeutic usefulness of these compounds is currently being investigated in a variety of disorders, including thrombosis (P2X1), chronic neuropathic and inflammatory pain (P2X3, P2X2/3, P2X4, P2X7), dysfunctional urinary bladder (P2X1, P2X3, P2X2/3), rheumatoid arthritis and osteoarthritis (P2X7), and depression (P2X7). 

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P2X4 receptors in activated C8-B4 cells of cerebellar microglial origin

Cited by 5 publications

References 61 publications

Involvement of P2X4 receptors in hippocampal microglial activation afterstatus epilepticus

Involvement of P2X4 receptors in hippocampal microglial activation afterstatus epilepticus

CNS-derived CCL21 is both sufficient to drive homeostatic CD4+ T cell proliferation and necessary for efficient CD4+ T cell migration into the CNS parenchyma following Toxoplasma gondii infection

Pharmacology of P2X receptors

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