Abstract

The Harvard Medical School and two of its geographically juxtaposed affiliated hospitals, the Beth Israel and Brigham and Women's, have joined to establish a digestive disease center whose major emphasis is the more effective study of relationships between structure and function in the alimentary tract. This theme emerged very clearly and naturally from the findings of an in-depth analysis of the strengths of the component institutions during the period of an exploratory grant awarded for the purpose of planning an integrated digestive diseases center. Each of the three institutions not only has strong programs in morphology at the cellular and molecular level, but there are also a large group of investigators with active programs to study function in the alimentary tract whose research is strongly potentiated by collaboration with morphologists. Furthermore, it has become increasingly evident that a variety of areas in alimentary tract research have suffered seriously in recent years because of inadequate correlations between structure and function. Interaction and collaboration between clinicians (gastroenterologists, surgeons, pathologists) and basic scientists will be emphasized. Several core resources serve to enhance the activities of the investigators. These include an administrative core, and resources for morphology, electrophysiology, lipid analysis and radioimmunoassay. An extensive enrichment program including the availability of grants for pilot-feasibility studies, weekly combined research conferences, annual symposia, and opportunities to spend short periods of time in selected laboratories outside our own institutions is currently ongoing. The long-term objectives of this center are to enhance our understanding and knowledge of digestive diseases, and thereby improve the care of patients with these conditions. We believe that this can be accomplished by furthering the interaction and collaboration of basic and clinical scientists working to expand the scope of physiological research with morphologic correlates, and vice versa.

  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 #
5P30DK034854-03
Application #
3102018
Study Section
(SRC)
Project Start
1984-09-30
Project End
1989-08-31
Budget Start
1986-09-01
Budget End
1987-08-31
Support Year
3
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Type
Schools of Medicine
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

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
Kotlarz, Daniel; Marquardt, Benjamin; Barøy, Tuva et al. (2018) Human TGF-?1 deficiency causes severe inflammatory bowel disease and encephalopathy. Nat Genet 50:344-348
Vardi, Iddo; Barel, Ortal; Sperber, Michal et al. (2018) Genetic and Structural Analysis of a SKIV2L Mutation Causing Tricho-hepato-enteric Syndrome. Dig Dis Sci 63:1192-1199
Garcia-Castillo, Maria Daniela; Chinnapen, Daniel J-F; Te Welscher, Yvonne M et al. (2018) Mucosal absorption of therapeutic peptides by harnessing the endogenous sorting of glycosphingolipids. Elife 7:
Basu, Sankha S; Delaney, Mary L; Li, Ning et al. (2018) Acetobacter indonesiensis Pneumonia after Lung Transplantation. Emerg Infect Dis 24:598-599
Yien, Yvette Y; Shi, Jiahai; Chen, Caiyong et al. (2018) FAM210B is an erythropoietin target and regulates erythroid heme synthesis by controlling mitochondrial iron import and ferrochelatase activity. J Biol Chem 293:19797-19811
Garber, John J; Mallick, Emily M; Scanlon, Karen M et al. (2018) Attaching-and-Effacing Pathogens Exploit Junction Regulatory Activities of N-WASP and SNX9 to Disrupt the Intestinal Barrier. Cell Mol Gastroenterol Hepatol 5:273-288
Maglic, Dejan; Schlegelmilch, Karin; Dost, Antonella Fm et al. (2018) YAP-TEAD signaling promotes basal cell carcinoma development via a c-JUN/AP1 axis. EMBO J 37:
Cho, Jin A; Lee, Ann-Hwee; Platzer, Barbara et al. (2018) Retraction Notice to: The Unfolded Protein Response Element IRE1? Senses Bacterial Proteins Invading the ER to Activate RIG-I and Innate Immune Signaling. Cell Host Microbe 23:571

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