Your search keyword '"Kurtoglu, Metin"' showing total 14 results

1. Preclinical evaluation of CD8+ anti-BCMA mRNA CAR T cells for treatment of multiple myeloma

Author

Lin, Liang, Cho, Shih-Feng, Xing, Lijie, Wen, Kenneth, Li, Yuyin, Yu, Tengteng, Hsieh, Phillip A., Chen, Hailin, Kurtoglu, Metin, Zhang, Yi, Andrew Stewart, C., Munshi, Nikhil, Anderson, Kenneth C., and Tai, Yu-Tzu

Abstract

Chimeric antigen receptor (CAR) T-cell therapy remains limited to select centers that can carefully monitor adverse events. To broaden use of CAR T cells in community clinics and in a frontline setting, we developed a novel CD8+ CAR T-cell product, Descartes-08, with predictable pharmacokinetics for treatment of multiple myeloma. Descartes-08 is engineered by mRNA transfection to express anti-BCMA CAR for a defined length of time. Descartes-08 expresses anti-BCMA CAR for 1 week, limiting risk of uncontrolled proliferation; produce inflammatory cytokines in response to myeloma target cells; and are highly cytolytic against myeloma cells regardless of the presence of myeloma-protecting bone marrow stromal cells, exogenous a proliferation-inducing ligand, or drug resistance including IMiDs. The magnitude of cytolysis correlates with anti-BCMA CAR expression duration, indicating a temporal limit in activity. In the mouse model of aggressive disseminated human myeloma, Descartes-08 induces BCMA CAR-specific myeloma growth inhibition and significantly prolongs host survival (p< 0.0001). These preclinical data, coupled with an ongoing clinical trial of Descartes-08 in relapsed/refractory myeloma (NCT03448978) showing preliminary durable responses and a favorable therapeutic index, have provided the framework for a recently initiated trial of an optimized/humanized version of Descartes-08 (i.e., Descartes-11) in newly diagnosed myeloma patients with residual disease after induction therapy.

Published

2021

2. Identification of Active Chemotherapy Regimens in Advanced Biliary Tract Carcinoma: A Review of Chemotherapy Trials in the past Two Decades

Author

Ulahannan, Susanna V, Rahma, Osama E, Duffy, Austin G, Makarova-Rusher, Oxana V, Kurtoglu, Metin, Liewehr, David J, Steinberg, Seth M, and Greten, Tim F

Abstract

SUMMARY Biliary tract carcinoma is a rare malignancy. We performed a comprehensive analysis of published prospective clinical trials in advanced biliary tract carcinoma in an attempt to identify active regimens in this setting. We searched PubMed and abstracts presented at the American Society of Clinical Oncology, Gastrointestinal Cancer Symposium, European Society of Medical Oncology and European Cancer Organization conferences for clinical trials in this disease. We found 83 trials. The effect of gemcitabine on overall survival benefit showed a strong trend (p = 0.014) and an improvement in progression-free survival (p = 0.003). Gemcitabine-based regimens containing 5-fluorouracil showed a trend toward an improved overall survival (p = 0.047) relative to platinum agents. Our findings support gemcitabine as the chemotherapy backbone for the treatment of patients with cholangiocarcinoma. Gemcitabine plus 5-fluorouracil combinations warrant further investigations.

Published

2015

3. Activation of the Unfolded Protein Response by 2-Deoxy-d-Glucose Inhibits Kaposi's Sarcoma-Associated Herpesvirus Replication and Gene Expression

Author

Leung, Howard J., Duran, Elda M., Kurtoglu, Metin, Andreansky, Samita, Lampidis, Theodore J., and Mesri, Enrique A.

Abstract

ABSTRACTLytic replication of the Kaposi's sarcoma-associated herpesvirus (KSHV) is essential for the maintenance of both the infected state and characteristic angiogenic phenotype of Kaposi's sarcoma and thus represents a desirable therapeutic target. During the peak of herpesvirus lytic replication, viral glycoproteins are mass produced in the endoplasmic reticulum (ER). Normally, this leads to ER stress which, through an unfolded protein response (UPR), triggers phosphorylation of the α subunit of eukaryotic initiation factor 2 (eIF2α), resulting in inhibition of protein synthesis to maintain ER and cellular homeostasis. However, in order to replicate, herpesviruses have acquired the ability to prevent eIF2α phosphorylation. Here we show that clinically achievable nontoxic doses of the glucose analog 2-deoxy-d-glucose (2-DG) stimulate ER stress, thereby shutting down eIF2α and inhibiting KSHV and murine herpesvirus 68 replication and KSHV reactivation from latency. Viral cascade genes that are involved in reactivation, including the master transactivator (RTA) gene, glycoprotein B, K8.1, and angiogenesis-regulating genes are markedly decreased with 2-DG treatment. Overall, our data suggest that activation of UPR by 2-DG elicits an early antiviral response via eIF2α inactivation, which impairs protein synthesis required to drive viral replication and oncogenesis. Thus, induction of ER stress by 2-DG provides a new antiherpesviral strategy that may be applicable to other viruses.

Published

2012

4. Distribution of Bim determines Mcl-1 dependence or codependence with Bcl-xL/Bcl-2 in Mcl-1–expressing myeloma cells

Author

Morales, Alejo A., Kurtoglu, Metin, Matulis, Shannon M., Liu, Jiangxia, Siefker, David, Gutman, Delia M., Kaufman, Jonathan L., Lee, Kelvin P., Lonial, Sagar, and Boise, Lawrence H.

Abstract

Dependence on Bcl-2 proteins is a common feature of cancer cells and provides a therapeutic opportunity. ABT-737 is an antagonist of antiapoptotic Bcl-2 proteins and therefore is a good predictor of Bcl-xL/Bcl-2 dependence. Surprisingly, analysis of Mcl-1–dependent multiple myeloma cell lines revealed codependence on Bcl-2/Bcl-xLin half the cells tested. Codependence is not predicted by the expression level of antiapoptotic proteins, rather through interactions with Bim. Consistent with these findings, acquired resistance to ABT-737 results in loss of codependence through redistribution of Bim to Mcl-1. Overall, these results suggest that complex interactions, and not simply expression patterns of Bcl-2 proteins, need to be investigated to understand Bcl-2 dependence and how to better use agents, such as ABT-737.

Published

2011

5. Distribution of Bim determines Mcl-1 dependence or codependence with Bcl-xL/Bcl-2 in Mcl-1–expressing myeloma cells

Author

Morales, Alejo A., Kurtoglu, Metin, Matulis, Shannon M., Liu, Jiangxia, Siefker, David, Gutman, Delia M., Kaufman, Jonathan L., Lee, Kelvin P., Lonial, Sagar, and Boise, Lawrence H.

Abstract

Dependence on Bcl-2 proteins is a common feature of cancer cells and provides a therapeutic opportunity. ABT-737 is an antagonist of antiapoptotic Bcl-2 proteins and therefore is a good predictor of Bcl-xL/Bcl-2 dependence. Surprisingly, analysis of Mcl-1–dependent multiple myeloma cell lines revealed codependence on Bcl-2/Bcl-xL in half the cells tested. Codependence is not predicted by the expression level of antiapoptotic proteins, rather through interactions with Bim. Consistent with these findings, acquired resistance to ABT-737 results in loss of codependence through redistribution of Bim to Mcl-1. Overall, these results suggest that complex interactions, and not simply expression patterns of Bcl-2 proteins, need to be investigated to understand Bcl-2 dependence and how to better use agents, such as ABT-737.

Published

2011

6. GHRH antagonist causes DNA damage leading to p21 mediated cell cycle arrest and apoptosis in human colon cancer cells

Author

Hohla, Florian, Buchholz, Stefan, Schally, Andrew V, Seitz, Stefan, Rick, Ferenc G., Szalontay, Luca, Varga, Jozsef L., Zarandi, Marta, Halmos, Gabor, Vidaurre, Irving, Krishan, Awtar, Kurtoglu, Metin, Chandna, Sudhir, Aigner, Elmar, and Datz, Christian

Abstract

We investigated the mechanisms of inhibitory effect of growth hormone-releasing hormone (GHRH) antagonist JMR-132 on the growth of HT29, HCT-116 and HCT-15 human colon cancer cells in vitro and in vivo.  High-affinity binding sites for GHRH and mRNA for GHRH and splice variant-1 (SV1) of the GHRH receptor were found in all three cell lines tested. Proliferation of HT-29, HCT-116 and HCT-15 cells was significantly inhibited in vitro by JMR-132. Time course studies revealed that the treatment of human HCT-116 colon cancer cells with 10μM GHRH antagonist JMR-132 causes a significant DNA damage as shown by an increase in olive tail moment (OTM) and loss of inner mitochondrial membrane potential (∆Ψm). Western blotting demonstrated a time-dependent increase in protein levels of phospho-p53 (Ser46), Bax, cleaved caspase-9, -3, cleavage of poly(ADP-ribose)polymerase (PARP) and a decrease in Bcl-2 levels. An augmentation in cell cycle checkpoint protein p21Waf1/Cip1 was accompanied by a cell cycle arrest in S-phase. DNA fragmentation visualized by the comet assay and the number of apoptotic cells increased time dependently as determined by flow cytometric annexinV and PI staining assays. In vivo, JMR-132 decreased the volume of HT-29, HCT-116 and HCT-15 tumors xenografted into athymic mice up to 75% (p

Published

2009

7. Preclinical Evaluation of CD8+ Anti-Bcma mRNA CAR T-Cells for the Control of Human Multiple Myeloma

Author

Lin, Liang, Xing, Lijie, Cho, Shih-Feng, Wen, Kenneth, Hsieh, Phillip A, Kurtoglu, Metin, Zhang, Yi, Stewart, C Andrew, Anderson, Kenneth C., and Tai, Yu-Tzu

Abstract

Kurtoglu: Cartesian Therapeutics: Employment. Zhang:Cartesian Therapeutics: Employment. Stewart:Cartesian Therapeutics: Employment. Anderson:Sanofi-Aventis: Other: Advisory Board; OncoPep: Other: Scientific founder ; C4 Therapeutics: Other: Scientific founder ; Gilead Sciences: Other: Advisory Board; Janssen: Other: Advisory Board.

Published

2019

8. Preclinical Evaluation of CD8+ Anti-Bcma mRNA CAR T-Cells for the Control of Human Multiple Myeloma

Author

Lin, Liang, Xing, Lijie, Cho, Shih-Feng, Wen, Kenneth, Hsieh, Phillip A, Kurtoglu, Metin, Zhang, Yi, Stewart, C Andrew, Anderson, Kenneth C., and Tai, Yu-Tzu

Abstract

Chimeric antigen receptor (CAR) T cells targeting BCMA are positioned to transform treatment of multiple myeloma (MM), and virally-generated anti-BCMA CAR T cells have shown impressive early stage clinical results. However, the safety risk/benefit, manufacturing constraints, and relevant patient populations of viral anti-BCMA CAR T have yet to be fully defined. Here we present preclinical characterization of an autologous mRNA-generated anti-BCMA CAR T cell product (Descartes-08) designed to reduce safety risk and broaden the fitness-for-use of anti-BCMA CAR T cell therapy. Descartes-08 are autologous CD8+ T cells that express anti-BCMA CAR on up to 90% of cells with duration of CAR expression for several days with subsequent reduction in expression to background approximately 1 week after their generation. The manufacturing process is clinically scalable with high purity and viability of Descartes-08 following cryopreservation. Descartes-08 undergo cytotoxic degranulation and produce cytokines IFNg, TNFα, IL-2, in response to multiple BCMA-expressing multiple myeloma target cell lines in an effector-to-target-ratio-dependent manner. Furthermore, Descartes-08 kills MM lines that are both resistant and sensitive to lenalidomide and pomalidomide, and/or MM cells that are grown in the presence of bone marrow stromal cells that clinically support MM survival. Moreover, Descartes-08 are highly cytotoxic against MM cells from both newly-diagnosed and relapsed patients. The magnitude of cytolytic and cytokine responses correlates with duration of anti-BCMA CAR expression and declines after 4 days, indicating a temporal limit in activity that is predicted to dramatically decrease the risk of severe cytokine release syndrome. In a mouse model of disseminated human MM, Descartes-08 shows CAR-specific suppression of myeloma that is maintained throughout the duration of treatment. Taken together, these results illustrate features of RNA-generated anti-BCMA CAR T cells that promise key clinical advantages, thereby supporting ongoing clinical development of Descartes-08 for treatment of MM (NCT03448978).

Published

2019

9. CD8+ Anti-BCMA mRNA CAR T-Cells Effectively Kill Human Multiple Myeloma Cells In Vitro and In Vivo

Author

Lin, Liang, Xing, Lijie, Acharya, Chirag M, Wen, Kenneth, Liu, Jiye, Hsieh, Phillip, Kurtoglu, Metin, Holderness, Jeffrey, Kalayoglu, Murat, Munshi, Nikhil, Richardson, Paul G, Anderson, Kenneth C, and Tai, Yu-Tzu

Abstract

Potent anti-multiple myeloma (MM) responses have been observed in early-stage clinical trials with virally-transduced chimeric antigen receptor (CAR) T-cells redirected to B-cell maturation antigen (BCMA), a membrane protein with extremely high sensitivity and specificity for MM and plasma cells. Despite significant potency, CAR T-cells engineered by virally-mediated gene transfer present a poor risk profile. Permanent modification enhances CAR persistence but also increases the risk of severe cytokine release syndrome (CRS), neurotoxicity, and prolonged plasma cell aplasia due to uncontrolled in vivoexpansion and long-term persistence of the permanently-modified CAR T-cells. In an effort to address these shortcomings while preserving efficacy, we have developed CD8+ anti-BCMA CAR T-cells modified transiently by mRNA transfection (Descartes-08). Descartes-08 manufactured at clinical scale showed high (>90%) purity, post-cryopreservation viability, and transfection efficiency. Descartes-08 demonstrated robust dose- and time- dependent killing of BCMA+ MM cell lines, including those with acquired resistance to immunomodulatory drugs (IMiDs), as well as primary MM cells co-cultured with autologous bone marrow stromal cells. Compared with transfected pan- (CD3+) anti-BCMA CAR T-cells, Descartes-08 (CD8+) demonstrated enhanced transfection and killing but reduced secretion of IFN-g, an inflammatory cytokine highly correlated with CRS. Descartes-08 also demonstrated robust dose-dependent efficacy in a disseminated human MM model (i.v. MM1SLuc cells in NSG mice), and could be safely administered repetitively to deepen responses. These results advocate for rapid clinical translation of Descartes-08, which may improve the benefit: risk profile of CAR T-cells in MM and enable their use in patients with earlier-stage disease.

Published

2017

10. Getting It Off Her Chest: A Case of an Anterior Mediastinal Mass

Author

Romelus, Amelie, Kurtoglu, Metin, and Diaz, Yvonne

Published

2013

11. Distribution of Bim Determines MCL-1 Dependence or Co-Dependence on BCL-xL/BCL-2 In Multiple Myeloma

Author

Boise, Lawrence H., Morales, Alejo A, Kurtoglu, Metin, Matulis, Shannon M, Markovitz, Rebecca, Lee, Kelvin P, and Lonial, Sagar

Abstract

Boise: University of Chicago: Patents & Royalties.

Published

2010

12. Distribution of Bim Determines MCL-1 Dependence or Co-Dependence on BCL-xL/BCL-2 In Multiple Myeloma

Author

Boise, Lawrence H., Morales, Alejo A, Kurtoglu, Metin, Matulis, Shannon M, Markovitz, Rebecca, Lee, Kelvin P, and Lonial, Sagar

Abstract

Abstract 4054

Published

2010

13. Displacement of Bim From Anti-Apoptotic Proteins Is the Primary Factor for Determining ABT-737 Activity in Multiple Myeloma Cell Lines.

Author

Morales, Alejo A, Kurtoglu, Metin, Siefker, David, Matulis, Shannon M, Gutman, Delia M, and Boise, Lawrence H.

Abstract

Boise: University of Chicago: Patents & Royalties.

Published

2009

14. Displacement of Bim From Anti-Apoptotic Proteins Is the Primary Factor for Determining ABT-737 Activity in Multiple Myeloma Cell Lines.

Author

Morales, Alejo A, Kurtoglu, Metin, Siefker, David, Matulis, Shannon M, Gutman, Delia M, and Boise, Lawrence H.

Abstract

Abstract 2851

Published

2009