Abstract

Bipolar Disorder is a major psychiatric disorder characterized by alternation between the extreme mood states of mania and depression. Many efficacious treatments exist; however, there is a high degree of variability in individual response. This frequently results in a lengthy trial and error process of treatment optimization which may take years. Lithium was the first mood stabilizing medication and is still the gold standard for treatment. Existing data suggests that lithium responsive bipolar disorder may be a distinct form of illness. There is a subset of patients who have a remarkably good response to lithium. These patients tend to have a family history of bipolar disorder and present with euphoric rather than irritable mania. Lithium response has also been shown to be familial. The goal of this project has been the identification of genes associated with response to lithium in bipolar disorder. In the last funding period, we studied a series of candidate genes in our retrospectively assessed sample of 184 patients. These studies found evidence for two genes predicting response to lithium. NTRK2 codes for the trkb receptor which is the receptor for BDNF also implicated in bipolar disorder. We found SNPs in the NTRK2 gene that were associated with response to lithium in those with euphoric mania but not associated in those with irritable mania. Conversely, the gene for the phosphodiesterase PDE11A was associated with response for all forms of mania. These data support the idea that lithium responsive bipolar disorder is genetically distinct. Retrospective data has numerous limitations. For this reason, we have also conducted a prospective clinical trial of lithium in bipolar disorder. Patients with bipolar disorder are first stabilized on lithium monotherapy over a three month period and then entered into the maintenance phase of the study. Patients are then followed for 2 years in order to detect relapse into mania or depression. SNPs are tested for association to response measured as time to relapse using a survival curve analysis. 75 subjects have entered the protocol to date. In this renewal, we propose to: 1) expand the retrospective sample to 500 subjects; 2) genotype the retrospective sample at an additional 50 genes; 3) recruit an additional 125 subjects into the prospective sample for a total of 200 and 4) replicate the most significant SNPs from the retrospective sample in the prospective sample.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01CX000363-05
Application #
8768440
Study Section
Mental Health and Behavioral Science A (MHBA)
Project Start
2010-10-01
Project End
2015-09-30
Budget Start
2014-10-01
Budget End
2015-09-30
Support Year
5
Fiscal Year
2015
Total Cost
Indirect Cost

  Institution

Name
VA San Diego Healthcare System
Department
Type
DUNS #
073358855
City
San Diego
State
CA
Country
United States
Zip Code
92161

  Publications

Luzum, J A; Pakyz, R E; Elsey, A R et al. (2017) The Pharmacogenomics Research Network Translational Pharmacogenetics Program: Outcomes and Metrics of Pharmacogenetic Implementations Across Diverse Healthcare Systems. Clin Pharmacol Ther 102:502-510
Mertens, Jerome; Wang, Qiu-Wen; Kim, Yongsung et al. (2016) Erratum: Differential responses to lithium in hyperexcitable neurons from patients with bipolar disorder. Nature 530:242
McCarthy, Michael J; Le Roux, Melissa J; Wei, Heather et al. (2016) Calcium channel genes associated with bipolar disorder modulate lithium's amplification of circadian rhythms. Neuropharmacology 101:439-48
Mertens, Jerome; Wang, Qiu-Wen; Kim, Yongsung et al. (2015) Differential responses to lithium in hyperexcitable neurons from patients with bipolar disorder. Nature 527:95-9
Manchia, Mirko; Adli, Mazda; Akula, Nirmala et al. (2013) Assessment of Response to Lithium Maintenance Treatment in Bipolar Disorder: A Consortium on Lithium Genetics (ConLiGen) Report. PLoS One 8:e65636
Leckband, S G; Kelsoe, J R; Dunnenberger, H M et al. (2013) Clinical Pharmacogenetics Implementation Consortium guidelines for HLA-B genotype and carbamazepine dosing. Clin Pharmacol Ther 94:324-8
Falcone, Mary; Smith, Ryan M; Chenoweth, Meghan J et al. (2013) Neuroimaging in psychiatric pharmacogenetics research: the promise and pitfalls. Neuropsychopharmacology 38:2327-37
McCarthy, Michael J; Nievergelt, Caroline M; Kelsoe, John R et al. (2012) A survey of genomic studies supports association of circadian clock genes with bipolar disorder spectrum illnesses and lithium response. PLoS One 7:e32091
Thorn, Caroline F; Leckband, Susan G; Kelsoe, John et al. (2011) PharmGKB summary: carbamazepine pathway. Pharmacogenet Genomics 21:906-10
McCarthy, M J; Nievergelt, C M; Shekhtman, T et al. (2011) Functional genetic variation in the Rev-Erb? pathway and lithium response in the treatment of bipolar disorder. Genes Brain Behav 10:852-61

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