Abstract

The overarching goal of the HDDC is to facilitate the discovery of basic mechanisms underlying digestive health and disease, and to encourage the translation of these basic discoveries to improvement in patient care. The Clinical and Translational Program (Clinical Component) of the HDDC is designed to support basic science by providing human materials to HDDC members who are conducting basic and translational laboratory research, and also to support the specialized needs of our collaborating ?Clinical Associates.? Our strategy is to facilitate and support collaborations between basic, translational, and clinical researchers, and to leverage resources currently in place at CHB and BWH, by ?buying in? to the BCH Bio-Repository & Harvard IBD Data Registry, the BWH Inflammatory Bowel Disease Tissue Repository (BrITR), and BCH/BWH Biostatistics Resources.
The Specific Aims of the HDDC Clinical and Translational Research Program are: 1. To forge collaborations between HDDC Clinical Associates and HDDC Members, thus assuring availability of fresh and stored human samples for basic and translational research, and guiding HDDC basic research advances toward potential clinical applications. 2. To support a well-organized infrastructure for acquisition and storage of clinical samples (with relevant clinical metadata) as a long-term resource for current and future studies on gastrointestinal and liver diseases and normal human digestive function. 3. To provide professional support in biostatistics and study design to HDDC members and Clinical Associates for effective design of clinical studies and appropriate analysis and interpretation of data. The Clinical and Translational Program is directed by Scott B Snapper, MD, PhD, Director of the Center for IBD within the GI Division at CHB and Director of IBD Research at BWH. The Program has established clear guidelines for prioritization of resources for HDDC members and Clinical Associates, including access to fresh or stored human samples and availability of biostatistical support personnel. The Program is heavily subsidized by non-HDDC grant support and institutional resources from the Divisions of GI at BCH and BWH.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Center Core Grants (P30)
Project #
5P30DK034854-34
Application #
9605290
Study Section
Special Emphasis Panel (ZDK1)
Project Start
Project End
Budget Start
2018-12-01
Budget End
2019-11-30
Support Year
34
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Boston Children's Hospital
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Gornati, Laura; Zanoni, Ivan; Granucci, Francesca (2018) Dendritic Cells in the Cross Hair for the Generation of Tailored Vaccines. Front Immunol 9:1484
Blumberg, Richard S; Lillicrap, David; IgG Fc Immune Tolerance Group (2018) Tolerogenic properties of the Fc portion of IgG and its relevance to the treatment and management of hemophilia Blood 131:2205-2214
Yao, Lina; Seaton, Sarah Craven; Ndousse-Fetter, Sula et al. (2018) A selective gut bacterial bile salt hydrolase alters host metabolism. Elife 7:
Haghighi, Alireza; Krier, Joel B; Toth-Petroczy, Agnes et al. (2018) An integrated clinical program and crowdsourcing strategy for genomic sequencing and Mendelian disease gene discovery. NPJ Genom Med 3:21
Lee, Christine K; Mitchell, Paul D; Raza, Roshan et al. (2018) Validation of Transient Elastography Cut Points to Assess Advanced Liver Fibrosis in Children and Young Adults: The Boston Children's Hospital Experience. J Pediatr 198:84-89.e2
Santus, William; Mingozzi, Francesca; Vai, Marina et al. (2018) Deep Dermal Injection As a Model of Candida albicans Skin Infection for Histological Analyses. J Vis Exp :
Stein, Richard R; Tanoue, Takeshi; Szabady, Rose L et al. (2018) Computer-guided design of optimal microbial consortia for immune system modulation. Elife 7:
Chen, Peng; Tao, Liang; Wang, Tianyu et al. (2018) Structural basis for recognition of frizzled proteins by Clostridium difficile toxin B. Science 360:664-669
Shaw, Kelly A; Cutler, David J; Okou, David et al. (2018) Genetic variants and pathways implicated in a pediatric inflammatory bowel disease cohort. Genes Immun :
Lyons, Jesse; Ghazi, Phaedra C; Starchenko, Alina et al. (2018) The colonic epithelium plays an active role in promoting colitis by shaping the tissue cytokine profile. PLoS Biol 16:e2002417

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