Abstract

The Hopkins Population Center (HPC) requests a five-year renewal, for years 24 to 28, of its NICHD P30 Population Research Center Core Grant. The HPC has a long and distinguished record as a research center focusing on both domestic and international population issues. Population research at Hopkins, dating back to the 1930s, has always had a distinctive public health perspective, linking biological science to behavioral science, and taking results from the laboratory onto the street. Today, the HPC supports research throughout the University on population-related topics as diverse as the impact of welfare reform on families, the effects of needle-sharing networks on the spread of sexually-transmitted disease (STDs), development of a barrier method of female contraception that would also protect against STDs, and the manner in which cells in the mammalian testis communicate with each other. The HPC is administratively located in the Johns Hopkins School of Hygiene and Public Health, among the preeminent centers for public health research and teaching in the world. The School of Hygiene and Public Health provides a behavioral and biological science link between the Medical School and the social science departments in the School of Arts and Sciences. The HPC facilitates and fosters research connections within and between these divisions of the University through the provision of essential research infrastructure. Continuation of P30 support for the Center for the period 1997-2002 will allow us to maintain the existing infrastructure offered to Center associates, to expand the range of services offered and to accommodate the expected increase in numbers of associates over the next five years. This proposal requests support for seven Cores: (1) Administration; (2) Computing; (3) Information Services; 94) Quantitative Sciences; (5) Sexually Transmitted Disease Diagnostics; (6) Morphology; and (7) Radioimmunoassay. Over the grant period, the HPC proposes to take advantage of rapidly-evolving technology and recent faculty appointments to expand and improve the Center's cores, and to increase integration and communication among them.

  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 #
5P30HD006268-25
Application #
2673372
Study Section
Special Emphasis Panel (ZHD1-PRG-G (06))
Project Start
1978-03-01
Project End
2002-06-30
Budget Start
1998-07-01
Budget End
1999-06-30
Support Year
25
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Miscellaneous
Type
Schools of Public Health
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Becker, Stan; Hossain, Mian B; Thomson, Elizabeth (2006) Disagreement in spousal reports of current contraceptive use in sub-Saharan Africa. J Biosoc Sci 38:779-96
Misra, Dawn P; Astone, Nan; Lynch, Courtney D (2005) Maternal smoking and birth weight: interaction with parity and mother's own in utero exposure to smoking. Epidemiology 16:288-93
Choi, Yoonjoung; Bishai, David; Hill, Kenneth (2005) Socioeconomic differentials in supplementation of vitamin A: evidence from the Philippines. J Health Popul Nutr 23:156-64
Kagaayi, Joseph; Dreyfuss, Michele L; Kigozi, Godfrey et al. (2005) Maternal self-medication and provision of nevirapine to newborns by women in Rakai, Uganda. J Acquir Immune Defic Syndr 39:121-4
Hinson, Ella R; Shone, Scott M; Zink, M Christine et al. (2004) Wounding: the primary mode of Seoul virus transmission among male Norway rats. Am J Trop Med Hyg 70:310-7
Beenhakker, Britta; Becker, Stan; Hires, Stephanie et al. (2004) Are partners available for post-abortion contraceptive counseling? A pilot study in a Baltimore City clinic. Contraception 69:419-23
Hanna, William F; Kerr, Candace L; Shaper, Joel H et al. (2004) Lewis X-containing neoglycoproteins mimic the intrinsic ability of zona pellucida glycoprotein ZP3 to induce the acrosome reaction in capacitated mouse sperm. Biol Reprod 71:778-89
Wisniewski, Amy B; Klein, Sabra L; Lakshmanan, Yegappen et al. (2003) Exposure to genistein during gestation and lactation demasculinizes the reproductive system in rats. J Urol 169:1582-6
Charron, Martin; DeCerbo, Joshua N; Wright, William W (2003) A GC-box within the proximal promoter region of the rat cathepsin L gene activates transcription in Sertoli cells of sexually mature rats. Biol Reprod 68:1649-56
Charron, Martin; Folmer, Janet S; Wright, William W (2003) A 3-kilobase region derived from the rat cathepsin L gene directs in vivo expression of a reporter gene in sertoli cells in a manner comparable to that of the endogenous gene. Biol Reprod 68:1641-8

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