Search

Your search keyword '"Dubinett S"' showing total 241 results
Start Over Author "Dubinett S"
241 results on '"Dubinett S"'

1. Targeting myeloid-derived suppressor cells augments antitumor activity against lung cancer

Author

Srivastava MK, Zhu L, Harris-White M, Huang M, St John M, Lee JM, Salgia R, Cameron RB, Strieter R, Dubinett S, and Sharma S

Subjects
Lung Cancer, MDSC, APC, NK and T cell Activation, Immune Therapy, Immunologic diseases. Allergy, RC581-607
Abstract

Minu K Srivastava,1,2 Li Zhu,1,2 Marni Harris-White,2 Min Huang,1–3 Maie St John,1,3 Jay M Lee,1,3 Ravi Salgia,4 Robert B Cameron,1,3,5 Robert Strieter,6 Steven Dubinett,1–3 Sherven Sharma1–31Department of Medicine, UCLA Lung Cancer Research Program, David Geffen School of Medicine at UCLA, Los Angeles, CA, 2Molecular Gene Medicine Laboratory, Veterans Affairs Greater Los Angeles Healthcare System, Los Angeles, CA, 3Jonsson Comprehensive Cancer Center, David Geffen School of Medicine at UCLA, Los Angeles, CA, 4Department of Medicine, University of Chicago, Chicago, IL, 5Department of Surgery, Veterans Affairs Greater Los Angeles Healthcare System, Los Angeles, CA, 6Department of Medicine, University of Virginia, Charlottesville, VA, USAAbstract: Lung cancer evades host immune surveillance by dysregulating inflammation. Tumors and their surrounding stromata produce growth factors, cytokines, and chemokines that recruit, expand, and/or activate myeloid-derived suppressor cells (MDSCs). MDSCs regulate immune responses and are frequently found in malignancy. In this review the authors discuss tumor-MDSC interactions that suppress host antitumor activities and the authors' recent findings regarding MDSC depletion that led to improved therapeutic vaccination responses against lung cancer. Despite the identification of a repertoire of tumor antigens, hurdles persist for immune-based anticancer therapies. It is likely that combined therapies that address the multiple immune deficits in cancer patients will be required for effective therapy. MDSCs play a major role in the suppression of T-cell activation and they sustain tumor growth, proliferation, and metastases. Regulation of MDSC recruitment, differentiation or expansion, and inhibition of the MDSC suppressive function with pharmacologic agents will be useful in the control of cancer growth and progression. Pharmacologic agents that regulate MDSCs may be more effective when combined with immunotherapies. Optimization of combined approaches that simultaneously downregulate MDSC suppressor pathways, restore APC immune-stimulating activity, and expand tumor-reactive T cells will be useful in improving therapy.Keywords: MDSCs, antigen-presenting cells, natural killer cell activation, T-cell activation, immunotherapy

Published
2012

3. Systematic quantitative characterization of cellular responses induced by multiple signals

Author

Al-Shyoukh, I, Yu, F, Feng, J, Yan, K, Dubinett, S, Ho, CM, Shamma, JS, and Sun, R

Abstract

Background: Cells constantly sense many internal and environmental signals and respond through their complex signaling network, leading to particular biological outcomes. However, a systematic characterization and optimization of multi-signal responses remains a pressing challenge to traditional experimental approaches due to the arising complexity associated with the increasing number of signals and their intensities.Results: We established and validated a data-driven mathematical approach to systematically characterize signal-response relationships. Our results demonstrate how mathematical learning algorithms can enable systematic characterization of multi-signal induced biological activities. The proposed approach enables identification of input combinations that can result in desired biological responses. In retrospect, the results show that, unlike a single drug, a properly chosen combination of drugs can lead to a significant difference in the responses of different cell types, increasing the differential targeting of certain combinations. The successful validation of identified combinations demonstrates the power of this approach. Moreover, the approach enables examining the efficacy of all lower order mixtures of the tested signals. The approach also enables identification of system-level signaling interactions between the applied signals. Many of the signaling interactions identified were consistent with the literature, and other unknown interactions emerged.Conclusions: This approach can facilitate development of systems biology and optimal drug combination therapies for cancer and other diseases and for understanding key interactions within the cellular network upon treatment with multiple signals. © 2011 Al-Shyoukh et al; licensee BioMed Central Ltd.

Published
2011

4. 1199TiP Phase I trial of in situ vaccination with autologous CCL21-modified dendritic cells (CCL21-DC) combined with pembrolizumab for advanced NSCLC

Author

Lisberg, A.E., primary, Liu, B., additional, Salehi-Rad, R., additional, Lee, J.M., additional, Tran, L., additional, Krysan, K., additional, Lim, R., additional, Dumitras, C., additional, Jiang, Z., additional, Abtin, F., additional, Suh, R., additional, Genshaft, S., additional, Oh, S., additional, Fishbein, G.A., additional, O'Higgins, C.M., additional, Greenwald, D., additional, Goldman, J.W., additional, Elashoff, D., additional, Garon, E.B., additional, and Dubinett, S., additional

Published
2022
Full Text
View/download PDF

5. P11.01 Phase I Trial of in Situ Vaccination With Autologous CCL21-Modified Dendritic Cells (CCL21-DC) Combined With Pembrolizumab for Advanced NSCLC

Author

Lisberg, A., primary, Liu, B., additional, Salehi-Rad, R., additional, Lee, J., additional, Tran, L., additional, Kostyantyn, K., additional, Lim, R., additional, Dumitras, C., additional, Jing, Z., additional, Abtin, F., additional, Suh, R., additional, Genshaft, S., additional, Fishbein, G., additional, Kaul, A., additional, Kahlon, K., additional, Ashouri, S., additional, Goldman, J., additional, Elashoff, D., additional, Garon, E., additional, and Dubinett, S., additional

Published
2021
Full Text
View/download PDF

8. A11 Blockade of Myeloid Suppressor Cells Overcomes the Anti-PD-1/PD-L1 Resistance in KRAS-Driven and LKB1-Deficient NSCLC

Author

Li, R., primary, Salehi-Rad, R., additional, Momcilovic, M., additional, Lim, R., additional, Ong, S., additional, Huang, Z., additional, Tran, L., additional, Zhe, J., additional, Paul, M., additional, Teitell, M., additional, Minna, J., additional, Krysan, K., additional, Shackelford, D., additional, Liu, B., additional, and Dubinett, S., additional

Published
2020
Full Text
View/download PDF

9. A27 Stage I Lung Adenocarcinoma Gene Expression Associated with Aggressive Histologic Features for Guiding Precision Surgery and Therapy

Author

Zhang, J., primary, Burks, E., additional, Sullivan, T., additional, Sands, J., additional, Regis, S., additional, McKee, B., additional, McKee, A., additional, Zhang, S., additional, Liu, H., additional, Liu, G., additional, Dubinett, S., additional, Spira, A., additional, Beane, J., additional, Rieger-Christ, K., additional, and Lenburg, M., additional

Published
2020
Full Text
View/download PDF

11. Tolerance and Determinant Hierarchy

Author

Schneider, S. C., primary, Deng, H.-K., additional, Rottinger, B., additional, Sharma, S., additional, Stolina, M., additional, Bonpane, C., additional, Miller, A., additional, Dubinett, S., additional, Kyewski, B., additional, and Sercarz, E., additional

Published
2007
Full Text
View/download PDF

13. EP1.04-20 Phase I Trial of in Situ Vaccination with Autologous CCL21-Modified Dendritic Cells (CCL21-DC) Combined with Pembrolizumab for Advanced NSCLC

Author

Lisberg, A., primary, Liu, B., additional, Salehi-Rad, R., additional, Lee, J.M., additional, Tran, L., additional, Krysan, K., additional, Li, R., additional, Lin, Y., additional, Tseng, A., additional, Abtin, F., additional, Suh, R., additional, Oh, S., additional, Aberle, D., additional, Winter, L., additional, Wallace, W.D., additional, Elashoff, D., additional, Garon, E., additional, Sharma, S., additional, and Dubinett, S., additional

Published
2019
Full Text
View/download PDF

14. MA15.06 Stage I Lung Adenocarcinoma Gene Expression Associated with Aggressive Histologic Features for Guiding Precision Surgery and Therapy

Author

Zhang, J., primary, Burks, E., additional, Sullivan, T., additional, Sands, J., additional, Regis, S., additional, Mckee, B., additional, Mckee, A., additional, Zhang, S., additional, Liu, H., additional, Liu, G., additional, Dubinett, S., additional, Spira, A., additional, Beane, J., additional, Christ, K., additional, and Lenburg, M., additional

Published
2019
Full Text
View/download PDF

17. P2.09-05 Evaluation of PD-L1-Stained Tumor Cells via the 22C3 and SP-142 Antibodies in Cohort of Patients Treated on KEYNOTE-001

Author

Lisberg, A., primary, Hu-Lieskovan, S., additional, Grogan, T., additional, Carroll, J., additional, Shintaku, P., additional, Han, M., additional, Slamon, D., additional, Dubinett, S., additional, Goldman, J., additional, Elashoff, D., additional, Hellmann, M., additional, Ribas, A., additional, and Garon, E., additional

Published
2018
Full Text
View/download PDF

19. P1.04-14 HLA B44 Supertype Associated with Less Favorable Neoantigen Binding in Non-Small Cell Lung Cancer Treated with Immunotherapy

Author

Cummings, A., primary, Lu, H., additional, Gukasyan, J., additional, Madrigal, J., additional, Carroll, J., additional, Bornazyan, K., additional, Jones, B., additional, Noor, Z., additional, Lisberg, A., additional, Goldman, J.W., additional, Hu-Lieskovan, S., additional, Dubinett, S., additional, and Garon, E., additional

Published
2018
Full Text
View/download PDF

22. International Association for the Study of Lung Cancer Computed Tomography Screening Workshop 2011 Report

Author

Field, John K, Smith, Robert A., Aberle, Denise R., Oudkerk, Matthijs, Baldwin, David R., Yankelevitz, David, Pedersen, Jesper Holst, Swanson, Scott James, Travis, William D., Wisbuba, Ignacio I., Noguchi, Masayuki, Mulshine, Jim L, Baldwin, D. R., Yankelevitz, D., Brambilla, C., Dubinett, S., Jett, J., Lam, S., Perez Altozano, J., Dirksen, A., Leong, S., Massion, P. P., Mazzone, P., Young Chul Kim, Carrozzi, Laura, Choon Taek Lee, Arenberg, D., Yung, R., and Miller, Y.

Subjects
Pulmonary and Respiratory Medicine, medicine.medical_specialty, Lung Neoplasms, Cost effectiveness, IASLC workshop 2011, Biopsy, medicine.medical_treatment, MEDLINE, SOCIETY, LOBECTOMY, CT screening, CT screening recommendations, Lung cancer, Radiology, Humans, Lung, Practice Guidelines as Topic, Societies, Medical, Early Detection of Cancer, Mass Screening, Tomography, Spiral Computed, Oncology, COST-EFFECTIVENESS, 03 medical and health sciences, 0302 clinical medicine, Medical, Cancer screening, medicine, MANAGEMENT, Medical physics, 030212 general & internal medicine, SMALL PULMONARY NODULES, Tomography, Mass screening, business.industry, Cancer, ADENOCARCINOMA, medicine.disease, 3. Good health, ADULT SMOKERS, 030220 oncology & carcinogenesis, Smoking cessation, Spiral Computed, National Lung Screening Trial, Societies, business, FOLLOW-UP, MULTIDISCIPLINARY CLASSIFICATION, CT
Abstract

The International Association for the Study of Lung Cancer (IASLC) Board of Directors convened a computed tomography (CT) Screening Task Force to develop an IASLC position statement, after the National Cancer Institute press statement from the National Lung Screening Trial showed that lung cancer deaths fell by 20%. The Task Force's Position Statement outlined a number of the major opportunities to further improve the CT screening in lung cancer approach, based on experience with cancer screening from other organ sites.The IASLC CT Screening Workshop 2011 further developed these discussions, which are summarized in this report. The recommendation from the workshop, and supported by the IASLC Board of Directors, was to set up the Strategic CT Screening Advisory Committee (IASLC-SSAC). The Strategic CT Screening Advisory Committee is currently engaging professional societies and organizations who are stakeholders in lung cancer CT screening implementation across the globe, to focus on delivering guidelines and recommendations in six specific areas: (i) identification of high-risk individuals for lung cancer CT screening programs; (ii) develop radiological guidelines for use in developing national screening programs; (iii) develop guidelines for the clinical work-up of "in-determinate nodules" resulting from CT screening programmers; (iv) guidelines for pathology reporting of nodules from lung cancer CT screening programs; (v) recommendations for surgical and therapeutic interventions of suspicious nodules identified through lung cancer CT screening programs; and (vi) integration of smoking cessation practices into future national lung cancer CT screening programs.

Published
2012

23. Genomic Landscape of Atypical Adenomatous Hyperplasia and Their Progression to Lung Adenocarcinomas

Author

Sivakumar, S., primary, San Lucas, F.A., additional, McDowell, T.L., additional, Lang, W., additional, Xu, L., additional, Fujimoto, J., additional, Zhang, J., additional, Wistuba, I.I., additional, Futreal, F.A., additional, Fukuoka, J., additional, Yatabe, Y., additional, Dubinett, S., additional, Spira, A., additional, Fowler, J., additional, Hawk, E., additional, Scheet, P., additional, and Kadara, H., additional

Published
2017
Full Text
View/download PDF

26. EngageUC: Developing an Efficient and Ethical Approach to Biobanking Research at the University of California

Author

Garrett, SB, Koenig, BA, Brown, A, Hult, JR, Boyd, EA, Dry, S, Dohan, D, Berglund, L, Dubinett, S, Firestein, G, Grady, D, Daniel Mercola, Johnston, SC, Sak, R, Cavaleri, G, Longstaff, H, and Burgess, M

Subjects
Biomedical Research, Informed Consent, Cardiovascular Medicine And Haematology, Oncology And Carcinogenesis, Universities, population, in collaboration with UC BRAID, patients, translational research, biorepositories, Other Medical And Health Sciences, Humans, General Clinical Medicine, Biological Specimen Banks
Abstract

© 2015 Wiley Periodicals, Inc.. Biorepositories, or biobanks, provide researchers with access to biological samples and associated data in support of translational research. Efficient operation and ethical stewardship of biobanks involves coordinated efforts among multiple stakeholders including researchers who manage and use the repository, institutional officials charged with its oversight, and patients and volunteers who contribute samples and data. As advancements in translational research increasingly involve more data derived from larger numbers of diverse samples, the size and governance challenges facing biorepositories have grown. We describe an approach to developing efficient and ethical biobank governance that includes all major stakeholders. This model provides a pathway for addressing the technical and ethical challenges that must be resolved to ensure biorepositories continue to support translational research.

Published
2015

28. Iκbα gene transfer is cytotoxic to squamous-cell lung cancer cells and sensitizes them to tumor necrosis factor-α-mediated cell death

Author

Batra, R. K., Guttridge, D. C., David Brenner, Dubinett, S. M., Baldwin, A. S., and Boucher, R. C.

Abstract

Current paradigms in cancer therapy suggest that activation of nuclear factor-κB (NF-κB) by a variety of stimuli, including some cytoreductive agents, may inhibit apoptosis. Thus, inhibiting NF-κB activation may sensitize cells to anticancer therapy, thereby providing a more effective treatment for certain cancers. E-1-deleted adenoviral (Ad) vectors encoding a "superrepressor" form of the NF-κB inhibitor IκBα (AdIκBαSR) or β-galactosidase (AdLacZ) were tested alone and in combination with tumor necrosis factor-α (TNF-α) in lung cancer cells for sensitization of the cells to death. Following transduction with AdIκBαSR, lung cancer cells expressed IκBαSR in a dose-dependent manner. Probing nuclear extracts of lung cancer cells with NF-κB-sequence-specific oligonucleotides indicated that there was a minimal amount of NF-κB in the nucleus at baseline and an expected and dramatic increase in nuclear NF-κB following exposure of cells to TNF-α. Control E-1-deleted AdLacZ did not promote NF-κB activation. Importantly, AdIκBαSR-mediated gene transfer resulted in the complete block of nuclear translocation of NF-κB by specific binding of its p65/relA component with transgenic IκBαSR. At the cellular level, transduction with AdIκBαSR resulted in increased cytotoxicity in lung cancer cells as opposed to transduction with equivalent doses of AdLacZ. In addition, whereas the parental cells were resistant to TNF-α-mediated cytotoxicity, IκBαSR-transduced cells could be sensitized to TNF-α. Consequently, AdIκBαSR transduction followed by exposure to TNF-α uniformly resulted in the death of non-small-cell lung cancer cells. These data suggest that novel approaches incorporating IκBα gene therapy may have a role in the treatment of lung cancer.

Published
1999
Full Text
View/download PDF

33. Randomized phase II study of erlotinib (E) alone or combined with fulvestrant (F) in previously treated patients with advanced non-small cell lung cancer (NSCLC).

Author

Garon, E. B., primary, Dubinett, S. M., additional, Hosmer, W., additional, Reckamp, K. L., additional, Kabbinavar, F. F., additional, Goodglick, L., additional, Marquez-Garban, D. C., additional, Stabile, L. P., additional, Siegfried, J., additional, and Pietras, R. J., additional

Published
2010
Full Text
View/download PDF

36. Interim safety analysis of a phase II study of erlotinib (E) alone or combined with fulvestrant (F) in previously treated patients with advanced non-small cell lung cancer (NSCLC)

Author

Garon, E. B., primary, Sadeghi, S., additional, Kabbinavar, F. F., additional, Reckamp, K. L., additional, Marquez-Garban, D. C., additional, Stabile, L. P., additional, Goodglick, L., additional, Dubinett, S. M., additional, Siegfried, J. M., additional, and Pietras, R. J., additional

Published
2008
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results