Your search keyword '"Komarck, Christine M."' showing total 4 results

1. Fluorescence Detection of Colonic Neoplasia Using a Novel Peptide.

Author

Joshi, Bishnu P., Miller, Sharon J., Komarck, Christine M., Turgeon, D.K., Appelman, Henry D., Liu, Zhongyao, and Wang, Thomas D.

Published

2011

2. S1720 The NF-KappaB Inhibitor Commd1 Controls Intestinal Inflammation.

Author

Li, Haiying, Komarck, Christine M., van de Sluis, Bart, Melton, Shelby D., Faubion, William A., Genta, Robert M., Klomp, Leo W., Wijmenga, Cisca, and Burstein, Ezra

Published

2010

3. Refining risk stratification for locoregional failure after chemoradiotherapy in human papillomavirus-associated oropharyngeal cancer.

Author

Vainshtein, Jeffrey M., Spector, Matthew E., McHugh, Jonathan B., Wong, Ka Kit, Walline, Heather M., Byrd, Serena A., Komarck, Christine M., Ibrahim, Mohannad, Stenmark, Matthew H., Prince, Mark E., Bradford, Carol R., Wolf, Gregory T., McLean, Scott, Worden, Francis P., Chepeha, Douglas B., Carey, Thomas, and Eisbruch, Avraham

Subjects

*RADIOTHERAPY, *CANCER chemotherapy, *CANCER radiotherapy, *PAPILLOMAVIRUS diseases, *OROPHARYNGEAL cancer, *BIOMARKERS, *IMAGING of cancer

Abstract

Summary: Background: To determine whether the addition of molecular and imaging biomarkers to established clinical risk factors could help predict locoregional failure (LRF) after chemoradiation in human papillomavirus (HPV)-related (+) oropharyngeal cancer (OPC) and improve patient selection for locoregional treatment de-intensification. Methods: HPV status was determined for 198 consecutive patients with stage III/IV OPC treated with definitive chemoradiation from 5/2003 to 10/2010. The impact of pre-therapy epidermal growth factor receptor (EGFR) overexpression; imaging biomarkers including primary tumor and nodal maximum standardized uptake values on FDG-PET, gross tumor volumes, and matted nodes; and clinical factors on LRF (including residual disease at adjuvant neck dissection) was assessed. Results: Primary tumors were HPV+ in 184 patients and HPV-negative in 14. EGFR overexpression was related to HPV-negative status and was univariately associated with LRF in the overall population, but was neither retained in the multivariate model after adjustment for HPV status, nor associated with LRF in HPV+ patients. Similarly, imaging biomarkers were univariately associated with LRF, but correlated with T-stage and/or N-stage and did not remain predictive in HPV+ patients after adjustment for T4- and N3-stages, which were the only significant predictors of LRF on multivariate analysis. Among HPV+ patients with non-T4- or N3-stages, only minimal smoking was associated with decreased LRF. Conclusions: The prognostic impact of EGFR overexpression and imaging biomarkers on LRF was predominantly related to their association with HPV-negative status and T- or N-stage, respectively. Among HPV+ OPC patients treated with uniform chemoradiation, only T4-stage, N3-stage, and smoking contributed to risk-stratification for LRF. [ABSTRACT FROM AUTHOR]

Published

2014

4. COMMD Proteins, a Novel Family of Structural and Functional Homologs of MURR1.

Author

Burstein, Ezra, Hoberg, Jamie E., Wilkinson, Amanda S., Rumble, Julie M., Csomos, Rebecca A., Komarck, Christine M., Maine, Gabriel N., Wilkinson, John C., Mayo, Marty W., and Duckett, Cohn S.

Subjects

*NF-kappa B, *TRANSCRIPTION factors, *DNA-binding proteins, *PROTEINS, *BIOMOLECULES, *BIOCHEMISTRY

Abstract

MURR1 is a multifunctional protein that inhibits nuclear factor κB (NF-κB), a transcription factor with pleiotropic functions affecting innate and adaptive immunity, apoptosis, cell cycle regulation, and oncogenesis. Here we report the discovery of a new family of proteins with homology to MURR1. These proteins form multimeric complexes and were identified in a biochemical screen for MURRl-associated factors. The family is defined by the presence of a conserved and unique motif termed the COMM (copper metabolism gene MURR1) domain, which functions as an interface for protein. protein interactions. Like MURR1, several of these factors also associate with and inhibit NF-κB. The proteins designated as COMMD or COMM domain containing 1–10 are extensively conserved in multicellular eukaryotic organisms and define a novel family of structural and functional homologs of MURR1. The prototype of this family, MURR1/COMMD1, suppresses NF-κB not by affecting nuclear translocation or binding of NF-κB to cognate motifs; rather, it functions in the nucleus by affecting the association of NF-κB with chromatin. [ABSTRACT FROM AUTHOR]

Published

2005