Investigating the role of p11 (S100A10) sequence variation in susceptibility to major depression

Ranjana Verma; David J. Cutler; Peter Holmans; James A. Knowles; Raymond R. Crowe; William A. Scheftner; Myrna M. Weissman; J. Raymond DePaulo; Douglas F. Levinson; James B. Potash

doi:10.1002/ajmg.b.30514

Investigating the role of p11 (S100A10) sequence variation in susceptibility to major depression

Ranjana Verma, David J. Cutler, Peter Holmans, James A. Knowles, Raymond R. Crowe, William A. Scheftner, Myrna M. Weissman, J. Raymond DePaulo, Douglas F. Levinson, James B. Potash

School of Medicine

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

Recent evidence suggests a potential role for the p11 gene in conferring risk to depressive disorders. p11 has been shown to influence serotonergic transmission, and its expression was found to be reduced in a mouse model of depression, as well as in post-mortem brain tissue from major depressive disorder (MDD) cases. In the present study, we tested for rare variants in p11 by resequencing promoter, exonic and flanking intronic regions in 176 MDD cases and 176 matched controls. We also assessed common variation by genotyping eight single nucleotide polymorphisms (SNPs), seven tag SNPs and one found through resequencing, in 641 cases and 650 controls. Resequencing revealed nine novel rare variants, including a missense mutation (Asp60Glu) observed in one case and one control, and four variants that occurred only in cases and not controls. The number of rare variants in cases did not exceed that expected by chance for the length of sequence analyzed, and also was not significantly greater than that observed in controls. Resequencing also identified two known SNPs, one (rs4845720) of which was significantly more frequent in cases than controls in the resequenced sample (3.1% vs. 0.9%, P = 0.03), though not in the larger sample (3% vs. 2%, P = 0.15). None of the tag SNPs showed any evidence of association. Our results do not support a major role for either common or rare p11 SNPs with MDD. Several limitations of the study are discussed.

Original language	English (US)
Pages (from-to)	1079-1082
Number of pages	4
Journal	American Journal of Medical Genetics, Part B: Neuropsychiatric Genetics
Volume	144
Issue number	8
DOIs	https://doi.org/10.1002/ajmg.b.30514
State	Published - Dec 5 2007

Keywords

Association
Major depression
P11
S100A10
Serotonin
Tag SNPs

ASJC Scopus subject areas

Genetics(clinical)
Psychiatry and Mental health
Cellular and Molecular Neuroscience

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10.1002/ajmg.b.30514

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Verma, R., Cutler, D. J., Holmans, P., Knowles, J. A., Crowe, R. R., Scheftner, W. A., Weissman, M. M., DePaulo, J. R., Levinson, D. F., & Potash, J. B. (2007). Investigating the role of p11 (S100A10) sequence variation in susceptibility to major depression. American Journal of Medical Genetics, Part B: Neuropsychiatric Genetics, 144(8), 1079-1082. https://doi.org/10.1002/ajmg.b.30514

Verma, R, Cutler, DJ, Holmans, P, Knowles, JA, Crowe, RR, Scheftner, WA, Weissman, MM, DePaulo, JR, Levinson, DF & Potash, JB 2007, 'Investigating the role of p11 (S100A10) sequence variation in susceptibility to major depression', American Journal of Medical Genetics, Part B: Neuropsychiatric Genetics, vol. 144, no. 8, pp. 1079-1082. https://doi.org/10.1002/ajmg.b.30514

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abstract = "Recent evidence suggests a potential role for the p11 gene in conferring risk to depressive disorders. p11 has been shown to influence serotonergic transmission, and its expression was found to be reduced in a mouse model of depression, as well as in post-mortem brain tissue from major depressive disorder (MDD) cases. In the present study, we tested for rare variants in p11 by resequencing promoter, exonic and flanking intronic regions in 176 MDD cases and 176 matched controls. We also assessed common variation by genotyping eight single nucleotide polymorphisms (SNPs), seven tag SNPs and one found through resequencing, in 641 cases and 650 controls. Resequencing revealed nine novel rare variants, including a missense mutation (Asp60Glu) observed in one case and one control, and four variants that occurred only in cases and not controls. The number of rare variants in cases did not exceed that expected by chance for the length of sequence analyzed, and also was not significantly greater than that observed in controls. Resequencing also identified two known SNPs, one (rs4845720) of which was significantly more frequent in cases than controls in the resequenced sample (3.1% vs. 0.9%, P = 0.03), though not in the larger sample (3% vs. 2%, P = 0.15). None of the tag SNPs showed any evidence of association. Our results do not support a major role for either common or rare p11 SNPs with MDD. Several limitations of the study are discussed.",

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AU - Verma, Ranjana

AU - Cutler, David J.

AU - Holmans, Peter

AU - Knowles, James A.

AU - Crowe, Raymond R.

AU - Scheftner, William A.

AU - Weissman, Myrna M.

AU - DePaulo, J. Raymond

AU - Levinson, Douglas F.

AU - Potash, James B.

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N2 - Recent evidence suggests a potential role for the p11 gene in conferring risk to depressive disorders. p11 has been shown to influence serotonergic transmission, and its expression was found to be reduced in a mouse model of depression, as well as in post-mortem brain tissue from major depressive disorder (MDD) cases. In the present study, we tested for rare variants in p11 by resequencing promoter, exonic and flanking intronic regions in 176 MDD cases and 176 matched controls. We also assessed common variation by genotyping eight single nucleotide polymorphisms (SNPs), seven tag SNPs and one found through resequencing, in 641 cases and 650 controls. Resequencing revealed nine novel rare variants, including a missense mutation (Asp60Glu) observed in one case and one control, and four variants that occurred only in cases and not controls. The number of rare variants in cases did not exceed that expected by chance for the length of sequence analyzed, and also was not significantly greater than that observed in controls. Resequencing also identified two known SNPs, one (rs4845720) of which was significantly more frequent in cases than controls in the resequenced sample (3.1% vs. 0.9%, P = 0.03), though not in the larger sample (3% vs. 2%, P = 0.15). None of the tag SNPs showed any evidence of association. Our results do not support a major role for either common or rare p11 SNPs with MDD. Several limitations of the study are discussed.

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Investigating the role of p11 (S100A10) sequence variation in susceptibility to major depression

Abstract

Keywords

ASJC Scopus subject areas

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