Abstract

This is a competitive renewal application for a Population Center Grant (P30) from the Oregon Regional Primate Research Center (ORPRC) that requests support for core services to enhance individual research units. To access these services, investigators are funded to study issues within NICHD goals. Support is requested for six cores; a Cell Culture (CC) Core to provide reagents and maintain stable transfectants, a Hormone Analysis (HA) Core to perform immunoassays, bioassays, and high-pressure liquid chromatography, a Morphology (MOR) Core to assist with tissue and cell processing, including suitable methods for immunocytochemistry and preparative in situ hybridization, a Molecular Biology (MB) Core to generate specific probes and train investigators in their appropriate uses, an In Vitro Fertilization-Experimental Embryology (IVF-EE) Core to assist researchers in recovery, storage, and utilization of simian gametes; blastocysts and support cells, and a core for program administration (ADM). Each specialty core is directed by an experienced investigator in the proposed technologies who stresses consistent quality, efficiency and timely performance. The detection and solution of technical problems occur rapidly and development of new methodologies are feasible, thereby facilitating individual research projects. Seventeen investigators (P.I.s) utilize the multipurpose cores in studies to understand and optimize reproductive health in both sexes, although many projects emphasize the female. Specific areas of active research include: neuroendocrine events influencing the hypophyseal-gonadal axis during sexual development and adulthood; endocrine physiology of the menstrual cycle and pregnancy; mechanisms of steroid hormone action in the brain and reproductive tract; genomic processes in peptide expression and in receptor function; paracrine factors in neural and reproductive tissues; in vitro and in vivo fertilization; and the importance of photoperiodicity and aging in reproductive health. A total of 20 funded and 15 pending grants in these research areas seek access to one or more cores. The existence of these facilities enhances collaboration among members of these units and prevents unnecessary duplication of equipment, personnel and technologies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Center Core Grants (P30)
Project #
2P30HD018185-11
Application #
2197596
Study Section
Population Research Committee (HDPR)
Project Start
1984-09-01
Project End
1999-03-31
Budget Start
1994-09-01
Budget End
1995-03-31
Support Year
11
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Oregon Regional Primate Research Center
Department
Type
DUNS #
City
Beaverton
State
OR
Country
United States
Zip Code
97006

  Publications

Bethea, C L; Reddy, A P (2015) Ovarian steroids regulate gene expression related to DNA repair and neurodegenerative diseases in serotonin neurons of macaques. Mol Psychiatry 20:1565-78
Rivera, H M; Bethea, C L (2012) Ovarian steroids increase spinogenetic proteins in the macaque dorsal raphe. Neuroscience 208:27-40
Dissen, G A; Lomniczi, A; Boudreau, R L et al. (2012) Targeted gene silencing to induce permanent sterility. Reprod Domest Anim 47 Suppl 4:228-32
Tachibana, Masahito; Sparman, Michelle; Ramsey, Cathy et al. (2012) Generation of chimeric rhesus monkeys. Cell 148:285-95
Lee, Hyo-Sang; Ma, Hong; Juanes, Rita Cervera et al. (2012) Rapid mitochondrial DNA segregation in primate preimplantation embryos precedes somatic and germline bottleneck. Cell Rep 1:506-15
Tachibana, Masahito; Ma, Hong; Sparman, Michelle L et al. (2012) X-chromosome inactivation in monkey embryos and pluripotent stem cells. Dev Biol 371:146-55
Sorwell, Krystina G; Kohama, Steven G; Urbanski, Henryk F (2012) Perimenopausal regulation of steroidogenesis in the nonhuman primate. Neurobiol Aging 33:1487.e1-13
Dorfman, Mauricio D; Kerr, Bredford; Garcia-Rudaz, Cecilia et al. (2011) Neurotrophins acting via TRKB receptors activate the JAGGED1-NOTCH2 cell-cell communication pathway to facilitate early ovarian development. Endocrinology 152:5005-16
Garcia-Rudaz, Cecilia; Dorfman, Mauricio; Nagalla, Srinivasa et al. (2011) Excessive ovarian production of nerve growth factor elicits granulosa cell apoptosis by setting in motion a tumor necrosis factor ?/stathmin-mediated death signaling pathway. Reproduction 142:319-31
Adams Waldorf, K M; Rubens, C E; Gravett, M G (2011) Use of nonhuman primate models to investigate mechanisms of infection-associated preterm birth. BJOG 118:136-44

Showing the most recent 10 out of 96 publications