Abstract

The mission of the Cell and Molecular Biology Training Program (CMB Training Program) at Case Western Reserve University School of Medicine (CWRU-SOM) is to provide trainees with a multidisciplinary conceptual and technical foundation for developing independent careers conducting transformative research in the biomedical sciences. Molecular cell biology in the 21st century is increasingly driven by technological advances and involves collaborative, multidisciplinary research that brings together structural, biochemical, molecular and cellular approaches. Therefore, the overarching goal of the CMB Training Program is to provide trainees with broad skills and the flexibility to keep pace with the opportunities and demands of contemporary science. Faculty members at CWRU-SOM offer outstanding expertise in the disciplines of biochemistry, molecular biology, genetics, pharmacology, pathology, and neurosciences. CMB Trainers are engaged in research representing five major themes that transcend traditional departmental and program boundaries: RNA Processing and Translational Regulation; Genome Structure and Regulation; Intracellular Signaling; Proteomics and Bioinformatics; and Cancer Molecular Biology. CMB Trainees have the opportunity to work on a range of research topics that advance our fundamental understanding of the cellular and molecular mechanisms driving biological processes. Students are supported early in their careers (years 2-3) when the thesis project is in its formative stages and specialization into individual PhD Programs occurs. The core of the training program is a broad and rigorous curriculum in cell and molecular biology, as well as bioinformatics and genomics in the context of biomedicine with an emphasis on quantitative skills. In addition to a unifying theme of coursework, research discussions, and ethics training, students also take elective courses in structural biology, stem cell biology, cell biology, genetics, genomics, proteomics, and metabolomics, depending on their career goals. Trainees are exposed to a range of modern technologies and concepts and their application in cell and molecular biology. They apply these concepts in a mentored research project culminating in peer-reviewed research publications, rigorous oral and written examinations, regular faculty advisory committee meetings, departmental seminars, and presentations at national meetings. Program-specific activities such as the CMB Trainer/Trainee Seminar Series and the CMB Symposium Series offer intensive research presentation and discussions that also broadly impact the biomedical research community of CWRU-SOM. The success of the CMB Training Program continues to be measured by peer-?reviewed research publications, timely progress toward the PhD, subsequent postdoctoral training at top institutions, and advancement into independent research positions in academia and industry.

Public Health Relevance

Mechanistic insights into the function of cells and macromolecules represent key information for developing therapies to combat human disease. The CMB Training Program is aimed at teaching young scientists how to obtain such information and to prepare them for scientific careers in academia, industry, government, and education.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Institutional National Research Service Award (T32)
Project #
2T32GM008056-35
Application #
9279337
Study Section
NIGMS Initial Review Group (TWD)
Program Officer
Salazar, Desiree Lynn
Project Start
1983-09-22
Project End
2020-06-30
Budget Start
2017-07-01
Budget End
2018-06-30
Support Year
35
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Guenther, Ulf-Peter; Weinberg, David E; Zubradt, Meghan M et al. (2018) The helicase Ded1p controls use of near-cognate translation initiation codons in 5' UTRs. Nature 559:130-134
Somoza, Rodrigo A; Correa, Diego; Labat, Ivan et al. (2018) Transcriptome-Wide Analyses of Human Neonatal Articular Cartilage and Human Mesenchymal Stem Cell-Derived Cartilage Provide a New Molecular Target for Evaluating Engineered Cartilage. Tissue Eng Part A 24:335-350
Smolko, Anne E; Shapiro-Kulnane, Laura; Salz, Helen K (2018) The H3K9 methyltransferase SETDB1 maintains female identity in Drosophila germ cells. Nat Commun 9:4155
Forrest, Megan E; Saiakhova, Alina; Beard, Lydia et al. (2018) Colon Cancer-Upregulated Long Non-Coding RNA lincDUSP Regulates Cell Cycle Genes and Potentiates Resistance to Apoptosis. Sci Rep 8:7324
Zhang, Meixiang; Ngo, Justine; Pirozzi, Filomena et al. (2018) Highly efficient methods to obtain homogeneous dorsal neural progenitor cells from human and mouse embryonic stem cells and induced pluripotent stem cells. Stem Cell Res Ther 9:67
Knappenberger, Andrew J; Grandhi, Sneha; Sheth, Reena et al. (2017) Phylogenetic sequence analysis and functional studies reveal compensatory amino acid substitutions in loop 2 of human ribonucleotide reductase. J Biol Chem 292:16463-16476
Hannigan, Molly M; Zagore, Leah L; Licatalosi, Donny D (2017) Ptbp2 Controls an Alternative Splicing Network Required for Cell Communication during Spermatogenesis. Cell Rep 19:2598-2612
Forrest, Megan E; Khalil, Ahmad M (2017) Review: Regulation of the cancer epigenome by long non-coding RNAs. Cancer Lett 407:106-112
Kenny, T C; Hart, P; Ragazzi, M et al. (2017) Selected mitochondrial DNA landscapes activate the SIRT3 axis of the UPRmt to promote metastasis. Oncogene 36:4393-4404
Athman, Jaffre J; Sande, Obondo J; Groft, Sarah G et al. (2017) Mycobacterium tuberculosis Membrane Vesicles Inhibit T Cell Activation. J Immunol 198:2028-2037

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