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P2X7 polymorphism and chronic lymphocytic leukaemia: lack of correlation with incidence, survival and abnormalities of chromosome 12

P2X7 polymorphism and chronic lymphocytic leukaemia: lack of correlation with incidence, survival and abnormalities of chromosome 12
P2X7 polymorphism and chronic lymphocytic leukaemia: lack of correlation with incidence, survival and abnormalities of chromosome 12
The P2X7 receptor, a plasma membrane ATP-gated ion channel that plays a role in lymphocyte apoptosis, has been suggested as an important contributory factor to the pathogenesis of chronic lymphocytic leukaemia (CLL). The P2X7 gene resides on chromosome 12 and is polymorphic in the population at large (1513A/C) with the A and C alleles encoding fully active and nonfunctional proteins, respectively. We have evaluated the significance of this polymorphism by genotyping 144 patients with CLL and 348 healthy controls using a tetraprimer ARMS assay. We found no significant difference in allele frequency between patients and controls. Although patients with the C allele (A/C heterozygotes or C/C homozygotes) had a marginally shorter survival than those who were homozygous for the A allele, this difference was not significant for either the patient group considered as a whole or for IgVH-mutated/unmutated subsets. Finally, no association was found between trisomy 12 and P2X7 genotype. We conclude that the influence, if any, of P2X7 genotype on susceptibility to CLL or clinical outcome is small.
plasma, alleles, epidemiology, polymerase chain reaction, survival analysis, genetics, human, aged, research support, humans, chronic, survival, trisomy, incidence, dna, genetic, genotype
0887-6924
2097-2100
Zhang, L.Y.
177f7b42-c68e-4e2a-988a-b87d77713ac2
Ibbotson, R.E.
300e87bd-1bf5-4be3-9b36-bd5844ed457f
Orchard, J.A.
534ac42d-aef9-4323-a7a4-130f6c514ccc
Gardiner, A.C.
3fdf7e69-2cbc-4693-9977-4f92829d5316
Seear, R.V.
262c17cd-c5b4-4054-a78c-ae1f8cd8a6f0
Chase, A.J.
a40a09c2-3073-4655-ba0b-a802e34914b5
Oscier, D.G.
c2620a1d-25bb-48f7-9651-f5d023636381
Cross, N.C.P.
f87650da-b908-4a34-b31b-d62c5f186fe4
Zhang, L.Y.
177f7b42-c68e-4e2a-988a-b87d77713ac2
Ibbotson, R.E.
300e87bd-1bf5-4be3-9b36-bd5844ed457f
Orchard, J.A.
534ac42d-aef9-4323-a7a4-130f6c514ccc
Gardiner, A.C.
3fdf7e69-2cbc-4693-9977-4f92829d5316
Seear, R.V.
262c17cd-c5b4-4054-a78c-ae1f8cd8a6f0
Chase, A.J.
a40a09c2-3073-4655-ba0b-a802e34914b5
Oscier, D.G.
c2620a1d-25bb-48f7-9651-f5d023636381
Cross, N.C.P.
f87650da-b908-4a34-b31b-d62c5f186fe4

Zhang, L.Y., Ibbotson, R.E., Orchard, J.A., Gardiner, A.C., Seear, R.V., Chase, A.J., Oscier, D.G. and Cross, N.C.P. (2003) P2X7 polymorphism and chronic lymphocytic leukaemia: lack of correlation with incidence, survival and abnormalities of chromosome 12. Leukemia, 17 (11), 2097-2100. (doi:10.1038/sj.leu.2403125).

Record type: Article

Abstract

The P2X7 receptor, a plasma membrane ATP-gated ion channel that plays a role in lymphocyte apoptosis, has been suggested as an important contributory factor to the pathogenesis of chronic lymphocytic leukaemia (CLL). The P2X7 gene resides on chromosome 12 and is polymorphic in the population at large (1513A/C) with the A and C alleles encoding fully active and nonfunctional proteins, respectively. We have evaluated the significance of this polymorphism by genotyping 144 patients with CLL and 348 healthy controls using a tetraprimer ARMS assay. We found no significant difference in allele frequency between patients and controls. Although patients with the C allele (A/C heterozygotes or C/C homozygotes) had a marginally shorter survival than those who were homozygous for the A allele, this difference was not significant for either the patient group considered as a whole or for IgVH-mutated/unmutated subsets. Finally, no association was found between trisomy 12 and P2X7 genotype. We conclude that the influence, if any, of P2X7 genotype on susceptibility to CLL or clinical outcome is small.

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More information

Published date: 14 August 2003
Keywords: plasma, alleles, epidemiology, polymerase chain reaction, survival analysis, genetics, human, aged, research support, humans, chronic, survival, trisomy, incidence, dna, genetic, genotype

Identifiers

Local EPrints ID: 60461
URI: http://eprints.soton.ac.uk/id/eprint/60461
ISSN: 0887-6924
PURE UUID: e20af9e7-1dd0-43af-8bb7-568720788fa9
ORCID for A.J. Chase: ORCID iD orcid.org/0000-0001-6617-9953
ORCID for N.C.P. Cross: ORCID iD orcid.org/0000-0001-5481-2555

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Date deposited: 08 Sep 2008
Last modified: 16 Mar 2024 03:23

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Contributors

Author: L.Y. Zhang
Author: R.E. Ibbotson
Author: J.A. Orchard
Author: A.C. Gardiner
Author: R.V. Seear
Author: A.J. Chase ORCID iD
Author: D.G. Oscier
Author: N.C.P. Cross ORCID iD

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