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Featured researches published by Derek O'Neil.


Molecular Human Reproduction | 2012

Association of mutations in the zona pellucida binding protein 1 (ZPBP1) gene with abnormal sperm head morphology in infertile men

Alexander N. Yatsenko; Derek O'Neil; Angshumoy Roy; Paola A. Arias-Mendoza; Ruihong Chen; Lata Murthy; Dolores J. Lamb; Martin M. Matzuk

Nearly 7% of men are afflicted by male infertility worldwide, and genetic factors are suspected to play a significant role in the majority of these patients. Although sperm morphology is an important parameter measured in the semen analysis, only a few genetic causes of teratozoospermia are currently known. The objective of this study was to define the association between alterations in the genes encoding the Golgi-associated PDZ- and coiled-coil motif containing protein (GOPC), the protein interacting with C kinase 1 (PICK1) and the acrosomal protein zona pellucida binding protein 1 (ZPBP1/sp38) with abnormal sperm head morphology in infertile men. Previous reports demonstrated that mice lacking Gopc, Pick1 and Zpbp1 are infertile due to abnormal head morphology. Herein, using our validated RNA-based method, we studied spermatozoal cDNA encoding the human GOPC, PICK1 and ZPBP1 genes in 381 teratozoospermic and 240 controls patients via direct sequencing. Among these genes, we identified missense and splicing mutations in the sperm cDNA encoding ZPBP1 in 3.9% (15/381) of men with abnormal sperm head morphology. These mutations were not observed in 240 matched controls and the dbSNP database (χ(2) = 9.3, P = 0.002). In contrast, statistically significant and functionally relevant mutations were not discovered in the GOPC and PICK1 genes. In our study ZPBP1 mutations are associated with abnormal sperm head morphology, defined according to strict criteria, resembling the mouse Zpbp1 null phenotype. We hypothesize that missense mutations exert a dominant-negative effect due to altered ZPBP1 protein folding and protein:protein interactions in the acrosome.


Molecular Genetics and Metabolism | 2013

Dysregulation of Npas2 leads to altered metabolic pathways in a murine knockout model

Derek O'Neil; Hector Mendez-Figueroa; Toni Ann Mistretta; Chunliu Su; Robert H. Lane; Kjersti Aagaard

In our primate model of maternal high fat diet exposure, we have described that fetal epigenomic modifications to the peripheral circadian Npas2 are associated with persistent alterations in fetal hepatic metabolism and non-alcoholic fatty liver. As the interaction of circadian response with metabolism is not well understood, we employed a murine knockout model to characterize the molecular mechanisms with which Npas2 reprograms the fetal hepatic metabolic response. cDNA was generated from Npas2-/- and +/+ (wild type) livers at day 2 (newborn) and at 25 weeks (adult) of life. Newborn samples were analyzed by exon array (n = 3/cohort). Independent pathway analysis software determined that the primary dysregulated pathway(s) in the Npas2-/- animals uniformly converged on lipid metabolism. Of particular interest, Ppargc1a, which integrates circadian and metabolism pathways, was significantly (p < .01) over expressed in newborn (1.7 fold) and adult (1.8 fold) Npas2-/- animals. These findings are consistent with an essential role for Npas2 in programming the peripheral circadian response and hepatic metabolism, which has not been previously described.


American Journal of Obstetrics and Gynecology | 2018

268: Expression of the fetal hepatic circadian gene Npas2 regulates weight gain following high fat diet (HFD) feeding

Derek O'Neil; Danielle Goodspeed; Pablo J. Gonzalez-Rodriguez; Valeria Melo; Cynthia Shope; Kjersti Aagaard


Fertility and Sterility | 2017

The hepatic expressed circadian gene Npas2 influences the metabolic response to a restricted feeding diet and the developing gut microbiome

Derek O'Neil; Christopher J. Stewart; Derrick Chu; Danielle Goodspeed; Pablo J. Gonzalez-Rodriguez; Kjersti Aagaard


American Journal of Obstetrics and Gynecology | 2017

119: Loss of the peripheral circadian regulator Npas2 in the maternal liver is associated with differential weight gain in offspring

Danielle Goodspeed; Derek O'Neil; Pablo Gonzalez; Cynthia Shope; Kjersti Aagaard


American Journal of Obstetrics and Gynecology | 2017

22: The hepatic expressed circadian gene, npas2, influences the developing got microbiome with restricted feeding

Derek O'Neil; Danielle Goodspeed; Derrick Chu; Christopher J. Stewart; Cynthia Shope; Kjersti Aagaard


American Journal of Obstetrics and Gynecology | 2017

121: Timing of the loss of hepatic Npas2 is associated with metabolic dysregulation under stress conditions

Danielle Goodspeed; Derek O'Neil; Pablo Gonzalez; Cynthia Shope; Kjersti Aagaard


American Journal of Obstetrics and Gynecology | 2017

255: The hepatic circadian gene npas2 regulates satiety and obesity in response to a high-fat diet

Derek O'Neil; Danielle Goodspeed; Cynthia Shope; Kjersti Aagaard


American Journal of Obstetrics and Gynecology | 2017

120: Fetal loss of hepatic Npas2 results in metabolic syndrome under metabolic stress

Danielle Goodspeed; Derek O'Neil; Pablo Gonzalez; Cynthia Shope; Kjersti Aagaard


American Journal of Obstetrics and Gynecology | 2017

122: Hepatic Npas2 is required for metabolic homeostasis under stress conditions

Danielle Goodspeed; Derek O'Neil; Pablo Gonzalez; Cynthia Shope; Kjersti Aagaard

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Kjersti Aagaard

Baylor College of Medicine

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Cynthia Shope

Baylor College of Medicine

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Pablo Gonzalez

Baylor College of Medicine

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Robert H. Lane

Medical College of Wisconsin

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Melissa Suter

Baylor College of Medicine

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Chunliu Su

Baylor College of Medicine

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Derrick Chu

Baylor College of Medicine

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