An Arg307 to Gln Polymorphism within the ATP-binding Site Causes Loss of Function of the Human P2X7 Receptor

Gu, Ben; Sluyter, Ronald; Skarratt, Kristen K.; Shemon, Anne N.; Dao-Ung, Lan-Phuong; Fuller, Stephen J.; Barden, Julian A.; Clarke, Alison L.; Petrou, Steven; Wiley, James S.

doi:10.1074/jbc.m313902200

Cited by 127 publications

(154 citation statements)

References 45 publications

(82 reference statements)

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“…Net dye uptake indicates the percentage dye uptake induced by BzATP with control (no BzATP treatment) subtracted. The data shown are representative of more than three independent experiments and two-tailed Student's t tests (unpaired) compared to Reference (R) yielded significance levels of <0.05(*), <0.01(**), or <0.001 (***) as shown in b-e of-function (H155Y and A166G) variations are located in the first cysteine-rich domain and only one loss-of-function SNP (R307Q) is at the C-terminus between the second cysteine-rich domain and second membrane-spanning domain (this study and references [57][58][59]). The large extracellular loop is believed to be responsible for ligandbinding and is quite conserved among the P2X receptors, although the fine structure of the ligand-binding pocket is still uncertain.…”

Section: Discussionmentioning

confidence: 74%

“…However, the majority of these have not been validated at the population genetic level and their functional effects are unclear. Five loss-of-function nonsynonymous allelic SNPs in P2X 7 have been described to date, of which three are located in the carboxy-terminal cytoplasmic tail (T357S, E496A, and I568N) and two are in the extracellular loop [54][55][56][57][58]. Cabrini et al have characterized the first gain-of-function polymorphism identified (H155Y) [59].…”

Section: Introductionmentioning

confidence: 99%

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Identification and characterization of a novel variant of the human P2X7 receptor resulting in gain of function

Sun

Chu

Singh

et al. 2009

Purinergic Signalling

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The P2X 7 receptor exhibits significant allelic polymorphism in humans, with both loss and gain of function variants potentially impacting on a variety of infectious and inflammatory disorders. At least five loss-offunction polymorphisms (G150R, R307Q, T357S, E496A, and I568N) and two gain-of-function polymorphisms (H155Y and Q460R) have been identified and characterized to date. In this study, we used RT-PCR cloning to isolate and characterize P2X 7 cDNA clones from human PBMCs and THP-1 cells. A previously unreported variant with substitutions of V80M and A166G was identified. When expressed in HEK293 cells, this variant exhibited heightened sensitivity to the P2X 7 agonist (BzATP) relative to the most frequent allele, as shown by pore formation measured by fluorescent dye uptake into cells. Mutational analyses showed that A166G alteration was critical for the gain-offunction change, while V80M was not. Full-length variants with multiple previously identified nonsynonymous SNPs (H155Y, H270R, A348T, and E496A) were also identified. Distinct functional phenotypes of the P2X 7 variants or mutants constructed with multiple polymorphisms were observed. Gain-of-function variations (A166G or H155Y) could not rescue the loss-of-function E496A polymorphism. Synergistic effects of the gain-of-function variations were also observed. We also identified the A348T alteration as a weak gain-of-function variant. Thus, these results identify the new gain-of-function variant A166G and demonstrate that multiple-gene polymorphisms contribute to functional phenotypes of the human P2X 7 receptor.Furthermore, the results demonstrate that the C-terminal of the cysteine-rich domain 1 of P2X 7 is critical for regulation of P2X 7 -mediated pore formation.

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Section: Discussionmentioning

confidence: 74%

Section: Introductionmentioning

confidence: 99%

Identification and characterization of a novel variant of the human P2X7 receptor resulting in gain of function

Sun

Chu

Singh

et al. 2009

Purinergic Signalling

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“…From the genetics perspective, there are two polymorphisms that lead to a null allele of the P2X7 gene, one of them affecting 1-2% of the Caucasian population, has already been reported (Gu et al, 2004;Skarratt et al, 2005). In addition, one polymorphism was proven to impair ATP-induced IL-1β release from human monocytes and one to affect normal trafficking of this receptor Wiley et al, 2003).…”

Section: P2x7 Receptor: a Possible Mediator Of Orthodontic Mechanotramentioning

confidence: 99%

“…P2X7R has also direct clinical relevance because there are many functional human polymorphisms in the P2X7R gene, which can induce different levels of affinity of these receptors to ATP. One of these polymorphisms, a null allele that occurs in 2% of the Caucasian population, is especially important because it results in reduced expression of the ion channel by 50% (Gu et al, 2004). It is hypothesized that variability in the expression of the P2X7R gene is an important factor in the individual variation to applied orthodontic loads.…”

Section: Orthodontic Mechanotransduction and The Role Of The P2x7 Recmentioning

confidence: 99%

Orthodontic mechanotransduction and the role of the P2X7 receptor

Viecilli

Katona

Chen

et al. 2009

American Journal of Orthodontics and Dentofacial Orthopedics

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DEDICATIONTo my parents, who have supported my education. iv ACKNOWLEDGMENTSOne of the most important things I have learned during my PhD is the necessity of the existence of a working network of people that can help you achieve your goals. The more effectively this network functions, the higher the chance you will achieve the goals quickly.I would first like to thank my parents, who have unconditionally supported my decision to abandon a profitable private practice in Orthodontics, and return to humble student conditions while aiming for a full time academic career.I also thank my girlfriend Laura Kruter who has (almost always) been ok with my, some might say, not very sane ideas. Sometimes they do turn out fine, though (like this "PhD" one).I can hardly think of anyone else that could have complemented my work and ideas during this Program as well as Dr. Thomas Katona. While I was passionately conditioned to an idea, he was always rational and careful. While I was sometimes furious with a shortcoming, he was always temperate and humorous. When I ran into his office with some news about a project, he would always listen and almost never seem too busy to see me. While I was working and something went wrong, he would listen and wonder with me about the "whys" and "hows", instead of telling me what to do or express disappointment. He was even subject to some of my home culinary experiments. I was extremely fortunate to find someone that thought about science the same way I did, and that actually helped me with my project instead of just telling me what to do. I felt like we worked as a team, and that helped to increase my motivation during my studies. The third part of this project tested the role of the P2X7 receptor in the dentoalveolar morphology of C57B/6 mice. P2X7R KO (knockout) mice were compared to C57B/6 WT to identify differences in a maxillary molar and bone. Tooth dimensions viii were measured and 3D bone morphometry was conducted. No statistically significant differences were found between the two mouse types. P2X7R does not have a major effect on alveolar bone or tooth morphology.The final part examines the role of the P2X7 receptor in a controlled biomechanical model. Orthodontic mechanotransduction was compared in wild-type (WT) and P2X7R knock-out (KO) mice. Using Finite Element Analysis, mouse mechanics were scaled to produce typical human stress levels. Relationships between the biological responses and the calculated stresses were statistically tested and compared.There were direct relationships between certain stress magnitudes and root resorption and bone formation. Hyalinization and root and bone resorption were different in WT and KO. Orthodontic responses are related to the principal stress patterns in the PDL and the P2X7 receptor plays a significant role in their mechanotransduction.

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“…4,5 In addition, the K þ ionophore, nigericin, has recently been shown to cause the release of IL-18 from human monocytes. 16 Given the central role of IL-18 in immunity and inflammation, the Glu 496 Ala polymorphism 11 and other, rarer loss-of-function polymorphisms in the P2X 7 receptor 23,24 may have clinical significance. Impaired ATPinduced release of IL-18 may play an important role in diseases where reduced or absent levels of IL-18 are known to increase susceptibility to mycobacteria and certain bacteria, and severity of septic arthritis and endotoxic shock.…”

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confidence: 99%

P2X7 receptor polymorphism impairs extracellular adenosine 5′-triphosphate-induced interleukin-18 release from human monocytes

2004

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Interleukin (IL)-18 is an important proinflammatory cytokine processed and released from cells of the monocyte lineage by activation of the P2X 7 receptor by extracellular adenosine 5 0 -triphosphate (ATP). We examined if a loss-of-function polymorphism of the human P2X 7 receptor (glutamic acid-496 to alanine) impairs this process. Using a whole blood-based assay, ATP-induced release of IL-18 from homozygous subjects after 120 min incubation with ATP was 42% of that from wildtype subjects. Moreover, the level of ATP-induced IL-18 release from lipopolysaccharide (LPS)-primed monocytes of homozygous subjects after 30 and 60 min incubation with ATP was 21 and 44%, respectively, of that from wild-type monocytes. Nigericin, a K þ ionophore, induced a similar release of IL-18 from monocytes of either genotype. ATP-induced ethidium þ uptake in LPS-primed, monocytes of homozygous subjects was only 11% of that in wild-type monocytes, while P2X 7 surface expression on LPS-primed, homozygous monocytes was 44% of that on wild-type monocytes.

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An Arg307 to Gln Polymorphism within the ATP-binding Site Causes Loss of Function of the Human P2X7 Receptor

Cited by 127 publications

References 45 publications

Identification and characterization of a novel variant of the human P2X7 receptor resulting in gain of function

Identification and characterization of a novel variant of the human P2X7 receptor resulting in gain of function

Orthodontic mechanotransduction and the role of the P2X7 receptor

P2X7 receptor polymorphism impairs extracellular adenosine 5′-triphosphate-induced interleukin-18 release from human monocytes

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