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Pamela L. Belmonte

Johns Hopkins University

Publishes on Genetic Associations and Epidemiology, Genetic Syndromes and Imprinting, Autism Spectrum Disorder Research. 6 papers and 1.1k citations.

6Publications
1.1kTotal Citations
Genetic Associations and EpidemiologyGenetic Syndromes and ImprintingAutism Spectrum Disorder ResearchChild and Adolescent Psychosocial and Emotional DevelopmentStress Responses and Cortisol

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Top publicationsby citations

A review of the evidence from family, twin and adoption studies for a genetic contribution to adult psychiatric disorders
Regina A. Shih, Pamela L. Belmonte, Peter P. Zandi|International Review of Psychiatry|2004
Cited by 338

Family, twin and adoption studies have provided major evidence for the role of genetics in numerous psychiatric disorders including obsessive-compulsive disorder, panic disorder, major depressive disorder, bipolar disorder, schizophrenia and Alzheimer's disease. As the search for patterns of inheritance and candidate genes of these complex disorders continues, we review relevant findings from quantitative genetic studies and outline the main challenges for the field of psychiatric genetics to focus on in order to more definitively establish the underpinnings of genetic and environmental influences of adult psychopathology.

Sex‐specific association of the reelin gene with bipolar disorder
Fernando S. Goes, Virginia L. Willour, Peter Zandi et al.|American Journal of Medical Genetics Part B Neuropsychiatric Genetics|2009
Cited by 67Open Access

The Reelin gene (RELN) encodes a secretory glycoprotein critical for brain development and synaptic plasticity. Post-mortem studies have shown lower Reelin protein levels in the brains of patients with schizophrenia and bipolar disorder (BP) compared with controls. In a recent genome-wide association study of schizophrenia, the strongest association was found in a marker within RELN, although this association was seen only in women. In this study, we investigated whether genetic variation in RELN is associated with BP in a large family sample. We genotyped 75 tagSNPs and 6 coding SNPs in 1,188 individuals from 318 nuclear families, including 554 affected offspring. Quality control measures, transmission-disequilibrium tests (TDTs), and empirical simulations were performed in PLINK. We found a significant overtransmission of the C allele of rs362719 to BP offspring (OR = 1.47, P = 5.9 x 10(-4)); this withstood empirical correction for testing of multiple markers (empirical P = 0.048). In a hypothesis-driven secondary analysis, we found that the association with rs362719 was almost entirely accounted for by overtransmission of the putative risk allele to affected females (OR(Female) = 1.79, P = 8.9 x 10(-5) vs. OR(Male) = 1.12, P = 0.63). These results provide preliminary evidence that genetic variation in RELN is associated with susceptibility to BP and, in particular, to BP in females. However, our findings should be interpreted with caution until further replication and functional assays provide convergent support.