Association between the CCR5 32-bp deletion allele and late onset of schizophrenia

H.B. Rasmussen; S. Timm; A.G. Wang; K. Soby; H. Lublin; Mogens Fenger; R. Hemmingsen; T Werge; Henrik Berg Rasmussen; Sally Timm; August G Wang; Karen Søeby; Henrik Lublin; Ralf Peter Arnfred Hemmingsen; Thomas Werge

doi:http://dx.doi.org/10.1176/appi.ajp.163.3.507

Association between the CCR5 32-bp deletion allele and late onset of schizophrenia

H.B. Rasmussen, S. Timm, A.G. Wang, K. Soby, H. Lublin, Mogens Fenger, R. Hemmingsen, T Werge, Henrik Berg Rasmussen, Sally Timm, August G Wang, Karen Søeby, Henrik Lublin, Ralf Peter Arnfred Hemmingsen, Thomas Werge

40 Citationer (Scopus)

Abstract

OBJECTIVE: The 32-bp deletion allele in chemokine receptor CCR5 has been associated with several immune-mediated diseases and might be implicated in schizophrenia as well. METHOD: The authors genotyped DNA samples from 268 schizophrenia patients and 323 healthy subjects. Age at first admission to a psychiatric hospital department served as a measure of disease onset. RESULTS: Patients and comparison subjects differed marginally in their genotype distribution, with a slightly higher frequency of the deletion allele seen in the patients. The authors found the deletion allele to be associated with higher age at first admission. After age at first admission was analyzed as a continuous variable, it was dichotomized using 40 years as the cutoff. With this approach the authors found that genotype distributions of patients with age at first admission above the cutoff (possible cases of late-onset schizophrenia) and healthy subjects differed significantly. This was reflected in an increased frequency of the deletion allele in the patient subgroup. Patients with ages at first admission below and above 40 years significantly differed in distribution of genotypes and alleles, with an overrepresentation of the deletion allele in the latter subgroup of patients. CONCLUSIONS: These findings suggest that the CCR5 32-bp deletion allele is a susceptibility factor for schizophrenia with late onset. Alternatively, the CCR5 32-bp deletion allele may act as a modifier by delaying the onset of schizophrenia without affecting the disease susceptibility.

Originalsprog	Engelsk
Tidsskrift	American Journal of Psychiatry
Vol/bind	163
Udgave nummer	3
Sider (fra-til)	507-11
Antal sider	5
ISSN	0002-953X
DOI	https://doi.org/10.1176/appi.ajp.163.3.507
Status	Udgivet - 2006

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http://dx.doi.org/10.1176/appi.ajp.163.3.507

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Rasmussen, H. B., Timm, S., Wang, A. G., Soby, K., Lublin, H., Fenger, M., Hemmingsen, R., Werge, T., Rasmussen, H. B., Timm, S., Wang, A. G., Søeby, K., Lublin, H., Hemmingsen, R. P. A., & Werge, T. (2006). Association between the CCR5 32-bp deletion allele and late onset of schizophrenia. American Journal of Psychiatry, 163(3), 507-11. https://doi.org/10.1176/appi.ajp.163.3.507

@article{84c5ef6d2daa4703bb13e1adf5358242,

title = "Association between the CCR5 32-bp deletion allele and late onset of schizophrenia",

abstract = "OBJECTIVE: The 32-bp deletion allele in chemokine receptor CCR5 has been associated with several immune-mediated diseases and might be implicated in schizophrenia as well. METHOD: The authors genotyped DNA samples from 268 schizophrenia patients and 323 healthy subjects. Age at first admission to a psychiatric hospital department served as a measure of disease onset. RESULTS: Patients and comparison subjects differed marginally in their genotype distribution, with a slightly higher frequency of the deletion allele seen in the patients. The authors found the deletion allele to be associated with higher age at first admission. After age at first admission was analyzed as a continuous variable, it was dichotomized using 40 years as the cutoff. With this approach the authors found that genotype distributions of patients with age at first admission above the cutoff (possible cases of late-onset schizophrenia) and healthy subjects differed significantly. This was reflected in an increased frequency of the deletion allele in the patient subgroup. Patients with ages at first admission below and above 40 years significantly differed in distribution of genotypes and alleles, with an overrepresentation of the deletion allele in the latter subgroup of patients. CONCLUSIONS: These findings suggest that the CCR5 32-bp deletion allele is a susceptibility factor for schizophrenia with late onset. Alternatively, the CCR5 32-bp deletion allele may act as a modifier by delaying the onset of schizophrenia without affecting the disease susceptibility.",

author = "H.B. Rasmussen and S. Timm and A.G. Wang and K. Soby and H. Lublin and Mogens Fenger and R. Hemmingsen and T Werge and Rasmussen, {Henrik Berg} and Sally Timm and Wang, {August G} and Karen S{\o}eby and Henrik Lublin and Hemmingsen, {Ralf Peter Arnfred} and Thomas Werge",

year = "2006",

doi = "http://dx.doi.org/10.1176/appi.ajp.163.3.507",

language = "English",

volume = "163",

pages = "507--11",

journal = "The American Journal of Psychiatry",

issn = "0002-953X",

publisher = "American Psychiatric Publishing, Inc.",

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}

TY - JOUR

T1 - Association between the CCR5 32-bp deletion allele and late onset of schizophrenia

AU - Rasmussen, H.B.

AU - Timm, S.

AU - Wang, A.G.

AU - Soby, K.

AU - Lublin, H.

AU - Fenger, Mogens

AU - Hemmingsen, R.

AU - Werge, T

AU - Rasmussen, Henrik Berg

AU - Timm, Sally

AU - Wang, August G

AU - Søeby, Karen

AU - Lublin, Henrik

AU - Hemmingsen, Ralf Peter Arnfred

AU - Werge, Thomas

PY - 2006

Y1 - 2006

N2 - OBJECTIVE: The 32-bp deletion allele in chemokine receptor CCR5 has been associated with several immune-mediated diseases and might be implicated in schizophrenia as well. METHOD: The authors genotyped DNA samples from 268 schizophrenia patients and 323 healthy subjects. Age at first admission to a psychiatric hospital department served as a measure of disease onset. RESULTS: Patients and comparison subjects differed marginally in their genotype distribution, with a slightly higher frequency of the deletion allele seen in the patients. The authors found the deletion allele to be associated with higher age at first admission. After age at first admission was analyzed as a continuous variable, it was dichotomized using 40 years as the cutoff. With this approach the authors found that genotype distributions of patients with age at first admission above the cutoff (possible cases of late-onset schizophrenia) and healthy subjects differed significantly. This was reflected in an increased frequency of the deletion allele in the patient subgroup. Patients with ages at first admission below and above 40 years significantly differed in distribution of genotypes and alleles, with an overrepresentation of the deletion allele in the latter subgroup of patients. CONCLUSIONS: These findings suggest that the CCR5 32-bp deletion allele is a susceptibility factor for schizophrenia with late onset. Alternatively, the CCR5 32-bp deletion allele may act as a modifier by delaying the onset of schizophrenia without affecting the disease susceptibility.

AB - OBJECTIVE: The 32-bp deletion allele in chemokine receptor CCR5 has been associated with several immune-mediated diseases and might be implicated in schizophrenia as well. METHOD: The authors genotyped DNA samples from 268 schizophrenia patients and 323 healthy subjects. Age at first admission to a psychiatric hospital department served as a measure of disease onset. RESULTS: Patients and comparison subjects differed marginally in their genotype distribution, with a slightly higher frequency of the deletion allele seen in the patients. The authors found the deletion allele to be associated with higher age at first admission. After age at first admission was analyzed as a continuous variable, it was dichotomized using 40 years as the cutoff. With this approach the authors found that genotype distributions of patients with age at first admission above the cutoff (possible cases of late-onset schizophrenia) and healthy subjects differed significantly. This was reflected in an increased frequency of the deletion allele in the patient subgroup. Patients with ages at first admission below and above 40 years significantly differed in distribution of genotypes and alleles, with an overrepresentation of the deletion allele in the latter subgroup of patients. CONCLUSIONS: These findings suggest that the CCR5 32-bp deletion allele is a susceptibility factor for schizophrenia with late onset. Alternatively, the CCR5 32-bp deletion allele may act as a modifier by delaying the onset of schizophrenia without affecting the disease susceptibility.

U2 - http://dx.doi.org/10.1176/appi.ajp.163.3.507

DO - http://dx.doi.org/10.1176/appi.ajp.163.3.507

M3 - Journal article

SN - 0002-953X

VL - 163

SP - 507

EP - 511

JO - The American Journal of Psychiatry

JF - The American Journal of Psychiatry

IS - 3

ER -

Association between the CCR5 32-bp deletion allele and late onset of schizophrenia

Abstract

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