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2. Gain in the short arm of chromosome 2 (2p+) induces gene overexpression and drug resistance in chronic lymphocytic leukemia: analysis of the central role of XPO1

Author

Cosson, A, Chapiro, E, Bougacha, N, Lambert, J, Herbi, L, Cung, H-A, Algrin, C, Keren, B, Damm, F, Gabillaud, C, Brunelle-Navas, M-N, Davi, F, Merle-Béral, H, Le Garff-Tavernier, M, Roos-Weil, D, Choquet, S, Uzunov, M, Morel, V, Leblond, V, Maloum, K, Lepretre, S, Feugier, P, Lesty, C, Lejeune, J, Sutton, L, Landesman, Y, Susin, S A, and Nguyen-Khac, F

Published
2017
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3. Prolonged XPO1 inhibition is essential for optimal antileukemic activity in NPM1-mutated AML

Author

Pianigiani, G., Gagliardi, A., Mezzasoma, F., Rocchio, F., Tini, V., Bigerna, B., Sportoletti, P., Caruso, S., Marra, A., Peruzzi, S., Petito, E., Spinozzi, G., Shacham, S., Landesman, Y., Quintarelli, C., Gresele, P., Locatelli, Franco, Martelli, M. P., Falini, B., Brunetti, L., Locatelli F. (ORCID:0000-0002-7976-3654), Pianigiani, G., Gagliardi, A., Mezzasoma, F., Rocchio, F., Tini, V., Bigerna, B., Sportoletti, P., Caruso, S., Marra, A., Peruzzi, S., Petito, E., Spinozzi, G., Shacham, S., Landesman, Y., Quintarelli, C., Gresele, P., Locatelli, Franco, Martelli, M. P., Falini, B., Brunetti, L., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NPM1 is the most frequently mutated gene in adults with acute myeloid leukemia (AML). The interaction between mutant NPM1 (NPM1c) and exportin-1 (XPO1) causes aberrant cytoplasmic dislocation of NPM1c and promotes the high expression of homeobox (HOX) genes, which is critical for maintaining the leukemic state of NPM1-mutated cells. Although there is a rationale for using XPO1 inhibitors in NPM1-mutated AML, selinexor administered once or twice per week did not translate into clinical benefit in patients with NPM1 mutations. Here, we show that this dosing strategy results in only a temporary disruption of the XPO1-NPM1c interaction, limiting the efficacy of selinexor. Because the second-generation XPO1 inhibitor eltanexor can be administered more frequently, we tested the antileukemic activity of prolonged XPO1 inhibition in NPM1-mutated AML models. Eltanexor caused irreversible HOX downregulation, induced terminal AML differentiation, and prolonged the survival of leukemic mice. This study provides essential information for the appropriate design of clinical trials with XPO1 inhibitors in NPM1-mutated AML.

Published
2022

7. The Nuclear Export Inhibitor Selinexor Inhibits Hypoxia Signaling Pathways And 3D Spheroid Growth Of Cancer Cells

Author

Depping R, von Fallois M, Landesman Y, and Kosyna FK

Subjects
tumor growth, hypoxia, HIF, XPO1, nuclear transport, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, selinexor
Abstract

Reinhard Depping,1 Moritz von Fallois,1,2 Yosef Landesman,3 Friederike Katharina Kosyna1 1Center for Structural and Cell Biology in Medicine, Institute of Physiology, Working Group Hypoxia, University of Lübeck, Lübeck D-23562, Germany; 2Clinic for Radiotherapy, University Hospital Schleswig-Holstein, Lübeck D-23562, Germany; 3Karyopharm Therapeutics, Newton, MA, USACorrespondence: Friederike Katharina KosynaCenter for Structural and Cell Biology in Medicine, Institute of Physiology, Working Group Hypoxia, University of Lübeck, Ratzeburger Allee 160, Lübeck D-23562, GermanyTel +49 451 3101 7322Fax +49 451 3101 7304Email friederike.kosyna@uni-luebeck.dePurpose: The nucleocytoplasmic transport of macromolecules is critical for both cell physiology and pathophysiology. Exportin 1 (XPO1), the major nuclear export receptor, is involved in the cellular adaptation to reduced oxygen availability by controlling the nuclear activity of the hypoxia-inducible factors (HIFs). Recently, a specific inhibitor of XPO1, selinexor (KPT-330), has been identified that inhibits nuclear export of cargo proteins by binding to the XPO1 cargo-binding pocket.Patients and methods: We used different cancer cell lines from human tissues and evaluated the physiological activity of selinexor on the hypoxia response pathway in two-dimensional (2D) monolayer cell cultures in quantitative real-time (qRT)-PCR experiments and luciferase reporter gene assays. A three-dimensional (3D) tumor spheroid culture model of MCF-7 breast cancer cells was established to analyze the effect of selinexor on 3D tumor spheroid structure, formation and viability.Results: Selinexor treatment reduces HIF-transcriptional activity and expression of the HIF-1 target gene solute carrier family 2 member 1 (SLC2A1). Moreover, 3D tumor spheroid structure, formation and viability are inhibited in response to selinexor-induced nuclear export inhibition.Conclusion: Here, we demonstrate the effect of specific XPO1-inhibition on the hypoxic response on the molecular level in 2D and 3D culture models of MCF-7 cells.Keywords: nuclear transport, HIF, hypoxia, XPO1, selinexor, tumor growth

Published
2019

8. Selinexor, bortezomib, and dexamethasone versus bortezomib and dexamethasone in previously treated multiple myeloma: Outcomes by cytogenetic risk

Author

Richard, S. Chari, A. Delimpasi, S. Simonova, M. Spicka, I. Pour, L. Kriachok, I. Dimopoulos, M.A. Pylypenko, H. Auner, H.W. Leleu, X. Usenko, G. Hajek, R. Benjamin, R. Dolai, T.K. Sinha, D.K. Venner, C.P. Garg, M. Stevens, D.A. Quach, H. Jagannath, S. Moreau, P. Levy, M. Badros, A. Anderson, L.D., Jr. Bahlis, N.J. Facon, T. Mateos, M.V. Cavo, M. Chang, H. Landesman, Y. Chai, Y. Arazy, M. Shah, J. Shacham, S. Kauffman, M.G. Grosicki, S. Richardson, P.G.

Abstract

In the phase 3 BOSTON study, patients with multiple myeloma (MM) after 1–3 prior regimens were randomized to once-weekly selinexor (an oral inhibitor of exportin 1 [XPO1]) plus bortezomib-dexamethasone (XVd) or twice-weekly bortezomib-dexamethasone (Vd). Compared with Vd, XVd was associated with significant improvements in median progression-free survival (PFS), overall response rate (ORR), and lower rates of peripheral neuropathy, with trends in overall survival (OS) favoring XVd. In BOSTON, 141 (35.1%) patients had MM with high-risk (presence of del[17p], t[4;14], t[14;16], or ≥4 copies of amp1q21) cytogenetics (XVd, n = 70; Vd, n = 71), and 261 (64.9%) exhibited standard-risk cytogenetics (XVd, n = 125; Vd, n = 136). Among patients with high-risk MM, median PFS was 12.91 months for XVd and 8.61 months for Vd (HR, 0.73 [95% CI, (0.4673, 1.1406)], p = 0.082), and ORRs were 78.6% and 57.7%, respectively (OR 2.68; p = 0.004). In the standard-risk subgroup, median PFS was 16.62 months for XVd and 9.46 months for Vd (HR 0.61; p = 0.004), and ORRs were 75.2% and 64.7%, respectively (OR 1.65; p = 0.033). The safety profiles of XVd and Vd in both subgroups were consistent with the overall population. These data suggest that selinexor can confer benefits to patients with MM regardless of cytogenetic risk. ClinicalTrials.gov identifier: NCT03110562. © 2021 The Authors. American Journal of Hematology published by Wiley Periodicals LLC.

Published
2021

9. Selinexor, bortezomib, and dexamethasone versus bortezomib and dexamethasone in previously treated multiple myeloma: Outcomes by cytogenetic risk

Author

Richard, S, Chari, A, Delimpasi, S, Simonova, M, Spicka, I, Pour, L, Kriachok, I, Dimopoulos, MA, Pylypenko, H, Auner, HW, Leleu, X, Usenko, G, Hajek, R, Benjamin, R, Dolai, TK, Sinha, DK, Venner, CP, Garg, M, Stevens, DA, Quach, H, Jagannath, S, Moreau, P, Levy, M, Badros, A, Anderson, LD, Bahlis, NJ, Facon, T, Mateos, MV, Cavo, M, Chang, H, Landesman, Y, Chai, Y, Arazy, M, Shah, J, Shacham, S, Kauffman, MG, Grosicki, S, Richardson, PG, Richard, S, Chari, A, Delimpasi, S, Simonova, M, Spicka, I, Pour, L, Kriachok, I, Dimopoulos, MA, Pylypenko, H, Auner, HW, Leleu, X, Usenko, G, Hajek, R, Benjamin, R, Dolai, TK, Sinha, DK, Venner, CP, Garg, M, Stevens, DA, Quach, H, Jagannath, S, Moreau, P, Levy, M, Badros, A, Anderson, LD, Bahlis, NJ, Facon, T, Mateos, MV, Cavo, M, Chang, H, Landesman, Y, Chai, Y, Arazy, M, Shah, J, Shacham, S, Kauffman, MG, Grosicki, S, and Richardson, PG

Abstract

In the phase 3 BOSTON study, patients with multiple myeloma (MM) after 1-3 prior regimens were randomized to once-weekly selinexor (an oral inhibitor of exportin 1 [XPO1]) plus bortezomib-dexamethasone (XVd) or twice-weekly bortezomib-dexamethasone (Vd). Compared with Vd, XVd was associated with significant improvements in median progression-free survival (PFS), overall response rate (ORR), and lower rates of peripheral neuropathy, with trends in overall survival (OS) favoring XVd. In BOSTON, 141 (35.1%) patients had MM with high-risk (presence of del[17p], t[4;14], t[14;16], or ≥4 copies of amp1q21) cytogenetics (XVd, n = 70; Vd, n = 71), and 261 (64.9%) exhibited standard-risk cytogenetics (XVd, n = 125; Vd, n = 136). Among patients with high-risk MM, median PFS was 12.91 months for XVd and 8.61 months for Vd (HR, 0.73 [95% CI, (0.4673, 1.1406)], p = 0.082), and ORRs were 78.6% and 57.7%, respectively (OR 2.68; p = 0.004). In the standard-risk subgroup, median PFS was 16.62 months for XVd and 9.46 months for Vd (HR 0.61; p = 0.004), and ORRs were 75.2% and 64.7%, respectively (OR 1.65; p = 0.033). The safety profiles of XVd and Vd in both subgroups were consistent with the overall population. These data suggest that selinexor can confer benefits to patients with MM regardless of cytogenetic risk. ClinicalTrials.gov identifier: NCT03110562.

Published
2021

10. The role of nuclear export in primary high-risk prostate cancer: A genomic analysis identifies XPO1 as potential therapeutic agent in high risk prostate cancer

Author

Moris, L., primary, Van Den Broeck, T., additional, Buerki, C., additional, Davicioni, E., additional, Everaerts, W., additional, Handle, F., additional, Helsen, C., additional, Jacquemyn, M., additional, Landesman, Y., additional, Soenen, S., additional, Daelemans, D., additional, Joniau, S., additional, and Claessens, F., additional

Published
2021
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11. FoxO-1 contributes to the efficacy of the combination of the XPO1 inhibitor selinexor and cisplatin in ovarian carcinoma preclinical models

Author

Corno, C, Stucchi, S, De Cesare, M, Carenini, N, Stamatakos, S, Ciusani, E, Minoli, L, Scanziani, E, Argueta, C, Landesman, Y, Zaffaroni, N, Gatti, L, Perego, P, Corno C., Stucchi S., De Cesare M., Carenini N., Stamatakos S., Ciusani E., Minoli L., Scanziani E., Argueta C., Landesman Y., Zaffaroni N., Gatti L., Perego P., Corno, C, Stucchi, S, De Cesare, M, Carenini, N, Stamatakos, S, Ciusani, E, Minoli, L, Scanziani, E, Argueta, C, Landesman, Y, Zaffaroni, N, Gatti, L, Perego, P, Corno C., Stucchi S., De Cesare M., Carenini N., Stamatakos S., Ciusani E., Minoli L., Scanziani E., Argueta C., Landesman Y., Zaffaroni N., Gatti L., and Perego P.

Abstract

The XPO1/CRM1 inhibitor selinexor (KPT-330), is currently being evaluated in multiple clinical trials as an anticancer agent. XPO1 participates in the nuclear export of FoxO-1, which we previously found to be decreased in platinum-resistant ovarian carcinoma. The aim of this study was to determine whether enriching FoxO-1 nuclear localization using selinexor would increase ovarian cancer cell sensitivity to cisplatin. Selinexor, as a single agent, displayed a striking antiproliferative effect in different ovarian carcinoma cell lines. A schedule-dependent synergistic effect of selinexor in combination with cisplatin was found in cisplatin-sensitive IGROV-1, the combination efficacy being more evident in sensitive than in the resistant cells. In IGROV-1 cells, the combination was more effective when selinexor followed cisplatin exposure. A modulation of proteins involved in apoptosis (p53, Bax) and in cell cycle progression (p21WAF1) was found by Western blotting. Selinexor-treated cells exhibited enriched FoxO-1 nuclear staining. Knock-down experiments with RNA interference indicated that FOXO1-silenced cells displayed a reduced sensitivity to selinexor. FOXO1 silencing also tended to reduce the efficacy of the drug combination at selected cisplatin concentrations. Selinexor significantly inhibited tumor growth, induced FoxO-1 nuclear localization and improved the efficacy of cisplatin in IGROV-1 xenografts. Taken together, our results support FoxO-1 as one of the key factors promoting sensitivity towards selinexor and the synergistic interaction between cisplatin and selinexor in ovarian carcinoma cells with selected molecular backgrounds, highlighting the need for treatment regimens tailored to the molecular tumor features.

Published
2018

12. Selinexor in patients with relapsed or refractory diffuse large B -cell lymphoma (SADAL): a single -arm, multinational, multicentre, open -label, phase 2 trial

Author

Kalakonda, N., Maerevoet, M., Cavallo, F., Follows, G., Goy, A., Vermaat, J.S.P., Casasnovas, O., Hamad, N., Zijlstra, J.M., Bakhshi, S., Bouabdallah, R., Choquet, S., Gurion, R., Hill, B., Jaeger, U., Sancho, J.M., Schuster, M., Thieblemont, C., Cruz, F. de la, Egyed, M., Mishra, S., Offner, F., Vassilakopoulos, T.P., Warzocha, K., McCarthy, D., Ma, X.W., Corona, K., Saint-Martin, J.R., Chang, H., Landesman, Y., Joshi, A., Wang, H.W., Shah, J., Shacham, S., Kauffman, M., Neste, E. van den, and Canales, M.A.

Abstract

Background Relapsed or refractory diffuse large B -cell lymphoma (DLBCL) is an aggressive cancer with a median overall survival of less than 6 months. We aimed to assess the response to single -agent selinexor, an oral selective inhibitor of nuclear export, in patients with relapsed or refractory DLBCL who had no therapeutic options of potential clinical benefit. Methods SADAL was a multicentre, multinational, open -label, phase 2b study done in 59 sites in 19 countries. Patients aged 18 years or older with pathologically confirmed diffuse large B -cell lymphoma, an Eastern Cooperative Oncology Group performance status of 2 or less, who had received two to five lines of previous therapies, and progressed after or were not candidates for autologous stem -cell transplantation were enrolled. Germinal centre B -cell or non -germinal centre B -cell tumour subtype and double or triple expressor status were determined by immunohistochemistry and double or triple hit status was determined by cytogenetics. Patients received 60 mg selinexor orally on days 1 and 3 weekly until disease progression or unacceptable toxicity. The study was initially designed to evaluate both 60 mg and 100 mg twice -weekly doses of selinexor; however, the 100 mg dose was discontinued in the protocol (version 7.0) on March 29, 2017, when an improved therapeutic window was observed at 60 mg. Primary outcome was overall response rate. The primary outcome and safety were assessed in all patients who received 60 mg selinexor under protocol version 6.0, or enrolled under protocol versions 7.0 or higher and received at least one dose of selinexor. This trial is registered at ClinicalTrials.gov, NCT02227251 (active but not enrolling). Findings Between Oct 21, 2015, and Nov 2, 2019, 267 patients were randomly assigned, with 175 allocated to the 60 mg group and 92 to the discontinued 100 mg group. 48 patients assigned to the 60 mg group were excluded due to enrolment before version 6.0 of the protocol; the remaining 127 patients received selinexor 60 mg and were included in analyses of primary outcome and safety. The overall response rate was 28% (36/127; 95% CI 20?7-37?0); 15 (12%) achieved a complete response and 21 (17%) a partial response. The most common grade 3-4 adverse events were thrombocytopenia (n=58), neutropenia (n=31), anaemia (n=28), fatigue (n=14), hyponatraemia (n=10), and nausea (n=8). The most common serious adverse events were pyrexia (n=9), pneumonia (n=6), and sepsis (n=6). There were no deaths judged as related to treatment with selinexor. Interpretation Single -drug oral selinexor induced durable responses and had a manageable adverse events profile in patients with relapsed or refractory DLBCL who received at least two lines of previous chemoimmunotherapy. Selinexor could be considered a new oral, non-cytotoxic treatment option in this setting.

Published
2020

14. Selinexor in patients with relapsed or refractory diffuse large B-cell lymphoma (SADAL): a single-arm, multinational, multicentre, open-label, phase 2 trial

Author

Kalakonda, N. Maerevoet, M. Cavallo, F. Follows, G. Goy, A. Vermaat, J.S.P. Casasnovas, O. Hamad, N. Zijlstra, J.M. Bakhshi, S. Bouabdallah, R. Choquet, S. Gurion, R. Hill, B. Jaeger, U. Sancho, J.M. Schuster, M. Thieblemont, C. De la Cruz, F. Egyed, M. Mishra, S. Offner, F. Vassilakopoulos, T.P. Warzocha, K. McCarthy, D. Ma, X. Corona, K. Saint-Martin, J.-R. Chang, H. Landesman, Y. Joshi, A. Wang, H. Shah, J. Shacham, S. Kauffman, M. Van Den Neste, E. Canales, M.A.

Abstract

Background: Relapsed or refractory diffuse large B-cell lymphoma (DLBCL) is an aggressive cancer with a median overall survival of less than 6 months. We aimed to assess the response to single-agent selinexor, an oral selective inhibitor of nuclear export, in patients with relapsed or refractory DLBCL who had no therapeutic options of potential clinical benefit. Methods: SADAL was a multicentre, multinational, open-label, phase 2b study done in 59 sites in 19 countries. Patients aged 18 years or older with pathologically confirmed diffuse large B-cell lymphoma, an Eastern Cooperative Oncology Group performance status of 2 or less, who had received two to five lines of previous therapies, and progressed after or were not candidates for autologous stem-cell transplantation were enrolled. Germinal centre B-cell or non-germinal centre B-cell tumour subtype and double or triple expressor status were determined by immunohistochemistry and double or triple hit status was determined by cytogenetics. Patients received 60 mg selinexor orally on days 1 and 3 weekly until disease progression or unacceptable toxicity. The study was initially designed to evaluate both 60 mg and 100 mg twice-weekly doses of selinexor; however, the 100 mg dose was discontinued in the protocol (version 7.0) on March 29, 2017, when an improved therapeutic window was observed at 60 mg. Primary outcome was overall response rate. The primary outcome and safety were assessed in all patients who received 60 mg selinexor under protocol version 6.0, or enrolled under protocol versions 7.0 or higher and received at least one dose of selinexor. This trial is registered at ClinicalTrials.gov, NCT02227251 (active but not enrolling). Findings: Between Oct 21, 2015, and Nov 2, 2019, 267 patients were randomly assigned, with 175 allocated to the 60 mg group and 92 to the discontinued 100 mg group. 48 patients assigned to the 60 mg group were excluded due to enrolment before version 6.0 of the protocol; the remaining 127 patients received selinexor 60 mg and were included in analyses of primary outcome and safety. The overall response rate was 28% (36/127; 95% CI 20·7–37·0); 15 (12%) achieved a complete response and 21 (17%) a partial response. The most common grade 3–4 adverse events were thrombocytopenia (n=58), neutropenia (n=31), anaemia (n=28), fatigue (n=14), hyponatraemia (n=10), and nausea (n=8). The most common serious adverse events were pyrexia (n=9), pneumonia (n=6), and sepsis (n=6). There were no deaths judged as related to treatment with selinexor. Interpretation: Single-drug oral selinexor induced durable responses and had a manageable adverse events profile in patients with relapsed or refractory DLBCL who received at least two lines of previous chemoimmunotherapy. Selinexor could be considered a new oral, non-cytotoxic treatment option in this setting. Funding: Karyopharm Therapeutics Inc. © 2020 Elsevier Ltd

Published
2020

15. Phase 2 study of the Exportin 1 inhibitor selinexor in patients with recurrent gynecological malignancies

Author

Vergote, I. B., Lund, B., Peen, U., Umajuridze, Z., Mau-Sorensen, M., Kranich, A., Van Nieuwenhuysen, E., Haslund, C., Nottrup, T., Han, S. N., Concin, N., Unger, T. J., Chai, Y., Au, N., Rashal, T., Joshi, A., Crochiere, M., Landesman, Y., Shah, J., Shacham, S., Kauffman, M., Mirza, M. R., Vergote, I. B., Lund, B., Peen, U., Umajuridze, Z., Mau-Sorensen, M., Kranich, A., Van Nieuwenhuysen, E., Haslund, C., Nottrup, T., Han, S. N., Concin, N., Unger, T. J., Chai, Y., Au, N., Rashal, T., Joshi, A., Crochiere, M., Landesman, Y., Shah, J., Shacham, S., Kauffman, M., and Mirza, M. R.

Abstract

Background: Selinexor is an oral inhibitor of the nuclear export protein Exportin 1 (XPO1) with demonstrated antitumor activity in solid and hematological malignancies. We evaluated the efficacy and safety of selinexor in heavily pretreated, recurrent gynecological malignancies. Methods: In this phase 2 trial, patients received selinexor (35 or 50 mg/m2 twice-weekly [BIW] or 50 mg/m2 once-weekly [QW]) in 4-week cycles. Primary endpoint was disease control rate (DCR) including complete response (CR), partial response (PR) or stable disease (SD) ≥12 weeks. Secondary endpoints were progression-free survival (PFS), overall survival (OS) and safety. Results: 114 patients with ovarian (N = 66), endometrial (N = 23) or cervical (N = 25) cancer were enrolled. Median number of prior regimens for ovarian, endometrial and cervical cancer was 6 (1–11), 2 (1–5), and 3 (1–6) respectively. DCR was 30% (ovarian 30%; endometrial 35%; cervical 24%), which included confirmed PRs in 8%, 9%, and 4% of patients with ovarian, endometrial, and cervical cancer respectively. Median PFS and OS for patients with ovarian, endometrial and cervical cancer were 2.6, 2.8 and 1.4 months, and 7.3, 7.0, and 5.0 months, respectively. Common Grade 3/4 adverse events (AEs) were thrombocytopenia (17%), fatigue (14%), anemia (10%), nausea (9%) and hyponatremia (9%). Patients with ovarian cancer receiving 50 mg/m2 QW had fewer high-grade AEs with similar efficacy as BIW treatment. Conclusions: Selinexor demonstrated single-agent activity and disease control in patients with heavily pretreated ovarian and endometrial cancers. Side effects were a function of dose level and treatment frequency, similar to previous reports, reversible and mitigated with supportive care.

Published
2020

18. Oral selinexor-dexamethasone for triple-class refractory multiple myeloma

Author

Chari, A. Vogl, D.T. Gavriatopoulou, M. Nooka, A.K. Yee, A.J. Huff, C.A. Moreau, P. Dingli, D. Cole, C. Lonial, S. Dimopoulos, M. Stewart, A.K. Richter, J. Vij, R. Tuchman, S. Raab, M.S. Weisel, K.C. Delforge, M. Cornell, R.F. Kaminetzky, D. Hoffman, J.E. Costa, L.J. Parker, T.L. Levy, M. Schreder, M. Meuleman, N. Frenzel, L. Mohty, M. Choquet, S. Schiller, G. Comenzo, R.L. Engelhardt, M. Illmer, T. Vlummens, P. Doyen, C. Facon, T. Karlin, L. Perrot, A. Podar, K. Kauffman, M.G. Shacham, S. Li, L. Tang, S. Picklesimer, C. Saint-Martin, J.-R. Crochiere, M. Chang, H. Parekh, S. Landesman, Y. Shah, J. Richardson, P.G. Jagannath, S.

Abstract

BACKGROUND Selinexor, a selective inhibitor of nuclear export compound that blocks exportin 1 (XPO1) and forces nuclear accumulation and activation of tumor suppressor proteins, inhibits nuclear factor κB, and reduces oncoprotein messenger RNA translation, is a potential novel treatment for myeloma that is refractory to current therapeutic options. METHODS We administered oral selinexor (80 mg) plus dexamethasone (20 mg) twice weekly to patients with myeloma who had previous exposure to bortezomib, carfilzomib, lenalidomide, pomalidomide, daratumumab, and an alkylating agent and had disease refractory to at least one proteasome inhibitor, one immunomodulatory agent, and daratumumab (triple-class refractory). The primary end point was overall response, defined as a partial response or better, with response assessed by an independent review committee. Clinical benefit, defined as a minimal response or better, was a secondary end point. RESULTS A total of 122 patients in the United States and Europe were included in the modified intention-to-treat population (primary analysis), and 123 were included in the safety population. The median age was 65 years, and the median number of previous regimens was 7; a total of 53% of the patients had high-risk cytogenetic abnormalities. A partial response or better was observed in 26% of patients (95% confidence interval, 19 to 35), including two stringent complete responses; 39% of patients had a minimal response or better. The median duration of response was 4.4 months, median progression-free survival was 3.7 months, and median overall survival was 8.6 months. Fatigue, nausea, and decreased appetite were common and were typically grade 1 or 2 (grade 3 events were noted in up to 25% of patients, and no grade 4 events were reported). Thrombocytopenia occurred in 73% of the patients (grade 3 in 25% and grade 4 in 33%). Thrombocytopenia led to bleeding events of grade 3 or higher in 6 patients. CONCLUSIONS Selinexor-dexamethasone resulted in objective treatment responses in patients with myeloma refractory to currently available therapies. (Funded by Karyopharm Therapeutics; STORM ClinicalTrials.gov number, NCT02336815. © 2019 Massachusetts Medical Society.

Published
2019

19. Drosophila nuclear lamin precursor Dm0 is translated from either of two developmentally regulated mRNA species apparently encoded by a single gene.

Author

Gruenbaum, Y, Landesman, Y, Drees, B, Bare, JW, Saumweber, H, Paddy, MR, Sedat, JW, Smith, DE, Benton, BM, and Fisher, PA

Subjects
Biological Sciences, Genetics, Biotechnology, Amino Acid Sequence, Animals, Base Sequence, Cloning, Molecular, DNA, Drosophila Proteins, Drosophila melanogaster, Female, Genes, Immunoassay, Lamins, Molecular Sequence Data, Nuclear Proteins, Nucleic Acid Hybridization, Protein Biosynthesis, Protein Precursors, RNA, Messenger, Sequence Homology, Nucleic Acid, Transcription, Genetic, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

A cDNA clone encoding a portion of Drosophila nuclear lamins Dm1 and Dm2 has been identified by screening a lambda-gt11 cDNA expression library using Drosophila lamin-specific monoclonal antibodies. Two different developmentally regulated mRNA species were identified by Northern blot analysis using the initial cDNA as a probe, and full-length cDNA clones, apparently corresponding to each message, have been isolated. In vitro transcription of both full-length cDNA clones in a pT7 transcription vector followed by in vitro translation in wheat germ lysate suggests that both clones encode lamin Dm0, the polypeptide precursor of lamins Dm1 and Dm2. Nucleotide sequence analyses confirm the impression that both cDNA clones code for the identical polypeptide, which is highly homologous with human lamins A and C as well as with mammalian intermediate filament proteins. The two clones differ in their 3'-untranslated regions. In situ hybridization of lamin cDNA clones to Drosophila polytene chromosomes shows only a single locus of hybridization at or near position 25F on the left arm of chromosome 2. Southern blot analyses of genomic DNA are consistent with the notion that a single or only a few highly similar genes encoding Drosophila nuclear lamin Dm0 exist in the genome.

Published
1988

21. Pharmacodynamic and genomic markers associated with response to the XPO1/CRM1 inhibitor selinexor (KPT-330): A report from the pediatric preclinical testing program

Author

Attiyeh, EF, Maris, JM, Lock, R, Reynolds, CP, Kang, MH, Carol, H, Gorlick, R, Kolb, EA, Keir, ST, Wu, J, Landesman, Y, Shacham, S, Lyalin, D, Kurmasheva, RT, Houghton, PJ, Smith, MA, Attiyeh, EF, Maris, JM, Lock, R, Reynolds, CP, Kang, MH, Carol, H, Gorlick, R, Kolb, EA, Keir, ST, Wu, J, Landesman, Y, Shacham, S, Lyalin, D, Kurmasheva, RT, Houghton, PJ, and Smith, MA

Abstract

Background: Selinexor (KPT-330) is an inhibitor of the major nuclear export receptor, exportin 1 (XPO1, also termed chromosome region maintenance 1, CRM1) that has demonstrated activity in preclinical models and clinical activity against several solid and hematological cancers. Procedures: Selinexor was tested against the Pediatric Preclinical Testing Program (PPTP) in vitro cell line panel at concentrations from 1.0 nM to 10 μM and against the PPTP in vivo xenograft panels administered orally at a dose of 10 mg/kg thrice weekly for 4 weeks. Results: Selinexor demonstrated cytotoxic activity in vitro, with a median relative IC50 value of 123 nM (range 13.0 nM to >10 μM). Selinexor induced significant differences in event-free survival (EFS) distribution in 29 of 38 (76%) of the evaluable solid tumor xenografts and in five of eight (63%) of the evaluable ALL xenografts. Objective responses (partial or complete responses, PR/CR) were observed for 4 of 38 solid tumor xenografts including Wilms tumor, medulloblastoma (n = 2), and ependymoma models. For the ALL panel, two of eight (25%) xenografts achieved either CR or maintained CR. Two responding xenografts had FBXW7 mutations at R465 and two had SMARCA4 mutations. Selinexor induced p53, p21, and cleaved PARP in several solid tumor models. Conclusions: Selinexor induced regression against several solid tumor and ALL xenografts and slowed tumor growth in a larger number of models. Pharmacodynamic effects for XPO1 inhibition were noted. Defining the relationship between selinexor systemic exposures in mice and humans will be important in assessing the clinical relevance of these results. Pediatr Blood Cancer © 2015 Wiley Periodicals, Inc.

Published
2016

23. Results of a phase 2 trial of selinexor, an oral selective inhibitor of nuclear export (SINE) in 114 patients with gynaecological cancers

Author

Vergote, I., primary, Lund, B., additional, Havsteen, H., additional, Ujmajuridze, Z., additional, Van Nieuwenhuysen, E., additional, Haslund, C., additional, Juhler-Nøttrup, T., additional, Neven, P., additional, Mau-Sørensen, M., additional, Berteloot, P., additional, Kranich, A., additional, Rashal, T., additional, Meade, J., additional, Landesman, Y., additional, Saint-Martin, J.-R., additional, Wright, G., additional, Crochiere, M., additional, Shacham, S., additional, Kauffman, M., additional, and Raza Mirza, M., additional

Published
2016
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24. Circulating tumor cell number predicts time to progression (TTP) in patients with heavily pretreated gynecological cancers treated with selinexor (SEL)

Author

Crochiere, M., primary, Vergote, I.B., additional, Lund, B., additional, Havsteen, H., additional, Ujmajuridze, Z., additional, Van Nieuwenhuysen, E., additional, Haslund, C., additional, Juhler-Nøttrup, T., additional, Mau-Sørensen, M., additional, Berteloot, P., additional, Kranich, A., additional, Meade, J., additional, Wright, G., additional, Shacham, E., additional, Rashal, T., additional, Saint-Martin, J.-R., additional, Shacham, S., additional, Kauffman, M., additional, Mirza, M. Raza, additional, and Landesman, Y., additional

Published
2016
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26. KPT-8602, a second-generation inhibitor of XPO1-mediated nuclear export, is well tolerated and highly active against AML blasts and leukemia-initiating cells

Author

Etchin, J, primary, Berezovskaya, A, additional, Conway, A S, additional, Galinsky, I A, additional, Stone, R M, additional, Baloglu, E, additional, Senapedis, W, additional, Landesman, Y, additional, Kauffman, M, additional, Shacham, S, additional, Wang, J C Y, additional, and Look, A T, additional

Published
2016
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27. Pharmacodynamic and genomic markers associated with response to the XPO1/CRM1 inhibitor selinexor (KPT-330): A report from the pediatric preclinical testing program

Author

Attiyeh, EF, Maris, JM, Lock, R, Reynolds, CP, Kang, MH, Carol, H, Gorlick, R, Kolb, EA, Keir, ST, Wu, J, Landesman, Y, Shacham, S, Lyalin, D, Kurmasheva, RT, Houghton, PJ, Smith, MA, Attiyeh, EF, Maris, JM, Lock, R, Reynolds, CP, Kang, MH, Carol, H, Gorlick, R, Kolb, EA, Keir, ST, Wu, J, Landesman, Y, Shacham, S, Lyalin, D, Kurmasheva, RT, Houghton, PJ, and Smith, MA

Abstract

© 2015 Wiley Periodicals, Inc.Background: Selinexor (KPT-330) is an inhibitor of the major nuclear export receptor, exportin 1 (XPO1, also termed chromosome region maintenance 1, CRM1) that has demonstrated activity in preclinical models and clinical activity against several solid and hematological cancers. Procedures: Selinexor was tested against the Pediatric Preclinical Testing Program (PPTP) in vitro cell line panel at concentrations from 1.0nM to 10μM and against the PPTP in vivo xenograft panels administered orally at a dose of 10mg/kg thrice weekly for 4 weeks. Results: Selinexor demonstrated cytotoxic activity in vitro, with a median relative IC50 value of 123nM (range 13.0nM to >10μM). Selinexor induced significant differences in event-free survival (EFS) distribution in 29 of 38 (76%) of the evaluable solid tumor xenografts and in five of eight (63%) of the evaluable ALL xenografts. Objective responses (partial or complete responses, PR/CR) were observed for 4 of 38 solid tumor xenografts including Wilms tumor, medulloblastoma (n=2), and ependymoma models. For the ALL panel, two of eight (25%) xenografts achieved either CR or maintained CR. Two responding xenografts had FBXW7 mutations at R465 and two had SMARCA4 mutations. Selinexor induced p53, p21, and cleaved PARP in several solid tumor models. Conclusions: Selinexor induced regression against several solid tumor and ALL xenografts and slowed tumor growth in a larger number of models. Pharmacodynamic effects for XPO1 inhibition were noted. Defining the relationship between selinexor systemic exposures in mice and humans will be important in assessing the clinical relevance of these results.

Published
2015

28. Activity of a selective inhibitor of nuclear export, selinexor (KPT-330), against AML-initiating cells engrafted into immunosuppressed NSG mice

Author

Etchin, J, primary, Montero, J, additional, Berezovskaya, A, additional, Le, B T, additional, Kentsis, A, additional, Christie, A L, additional, Conway, A S, additional, Chen, W C, additional, Reed, C, additional, Mansour, M R, additional, Ng, C E L, additional, Adamia, S, additional, Rodig, S J, additional, Galinsky, I A, additional, Stone, R M, additional, Klebanov, B, additional, Landesman, Y, additional, Kauffman, M, additional, Shacham, S, additional, Kung, A L, additional, Wang, J C Y, additional, Letai, A, additional, and Look, A T, additional

Published
2015
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31. 247 Selective inhibitors of nuclear export (SINE) block the expression of DNA damage repair proteins and sensitize cancer cells to DNA damage therapeutic agents

Author

Kashyap, T., primary, Crochiere, M., additional, Friedlander, S., additional, Klebanov, B., additional, Senapedis, W., additional, Baloglu, E., additional, del Alamo, D., additional, Tamir, S., additional, Rashal, T., additional, McCauley, D., additional, Carlson, R., additional, Kauffman, M., additional, Shacham, S., additional, and Landesman, Y., additional

Published
2014
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33. Clinical Activity of the Oral Selective Inhibitor of Nuclear Export (Sine) Selinexor (Kpt-330) in Patients with Head & Neck Squamos Cell Carcinoma (Hn-Scc)

Author

Mahipal, A., primary, Gabrail, N.Y., additional, Sukari, A., additional, Mahaseth, H., additional, Mau-Sorensen, M., additional, Shacham, S., additional, Saint-Martin, J., additional, Friedlander, S., additional, Landesman, Y., additional, Ellis, J., additional, Shacham, E., additional, McCartney, J., additional, Marshall, T., additional, Vincent, D., additional, Rashal, T., additional, Kauffman, M., additional, Mirza, M.R., additional, and Razak, A.R.A., additional

Published
2014
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35. 886P - Circulating tumor cell number predicts time to progression (TTP) in patients with heavily pretreated gynecological cancers treated with selinexor (SEL)

Author

Crochiere, M., Vergote, I.B., Lund, B., Havsteen, H., Ujmajuridze, Z., Van Nieuwenhuysen, E., Haslund, C., Juhler-Nøttrup, T., Mau-Sørensen, M., Berteloot, P., Kranich, A., Meade, J., Wright, G., Shacham, E., Rashal, T., Saint-Martin, J.-R., Shacham, S., Kauffman, M., Mirza, M. Raza, and Landesman, Y.

Published
2016
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36. 854O - Results of a phase 2 trial of selinexor, an oral selective inhibitor of nuclear export (SINE) in 114 patients with gynaecological cancers

Author

Vergote, I., Lund, B., Havsteen, H., Ujmajuridze, Z., Van Nieuwenhuysen, E., Haslund, C., Juhler-Nøttrup, T., Neven, P., Mau-Sørensen, M., Berteloot, P., Kranich, A., Rashal, T., Meade, J., Landesman, Y., Saint-Martin, J.-R., Wright, G., Crochiere, M., Shacham, S., Kauffman, M., and Raza Mirza, M.

Published
2016
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37. O10 CRM1-selective inhibitors of nuclear export (sine) reduce the incidence of tumor spreading and improve overall survival in preclinical models of prostate cancer

Author

Festuccia, C., primary, Tortoreto, M., additional, Mancini, A., additional, Muzi, P., additional, Ventura, L., additional, Addis, A., additional, Landesman, Y., additional, Mccauley, D., additional, Kauffman, M., additional, Shacham, S., additional, Zaffaroni, N., additional, and Gravina, G., additional

Published
2013
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38. CRM1 inhibition induces tumor cell cytotoxicity and impairs osteoclastogenesis in multiple myeloma: molecular mechanisms and therapeutic implications

Author

Tai, Y-T, primary, Landesman, Y, additional, Acharya, C, additional, Calle, Y, additional, Zhong, M Y, additional, Cea, M, additional, Tannenbaum, D, additional, Cagnetta, A, additional, Reagan, M, additional, Munshi, A A, additional, Senapedis, W, additional, Saint-Martin, J-R, additional, Kashyap, T, additional, Shacham, S, additional, Kauffman, M, additional, Gu, Y, additional, Wu, L, additional, Ghobrial, I, additional, Zhan, F, additional, Kung, A L, additional, Schey, S A, additional, Richardson, P, additional, Munshi, N C, additional, and Anderson, K C, additional

Published
2013
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44. Selinexor, bortezomib, and dexamethasone versus bortezomib and dexamethasone in previously treated multiple myeloma: Outcomes by cytogenetic risk

Author

Hua Chang, Nizar J. Bahlis, Jatin P. Shah, Yi Chai, Shambavi Richard, Sosana Delimpasi, Ganna Usenko, Halyna Pylypenko, Meletios A. Dimopoulos, Holger W. Auner, Don A. Stevens, Ajai Chari, Reuben Benjamin, Melina Arazy, Moshe Yair Levy, Tuphan Kanti Dolai, Ivan Spicka, Hang Quach, Larry D. Anderson, Paul G. Richardson, Xavier Leleu, Maria-Victoria Mateos, Ashraf Z. Badros, Sharon Shacham, Iryna Kriachok, Thierry Facon, Roman Hájek, Sebastian Grosicki, Maryana Simonova, Ludek Pour, Yosef Landesman, Christopher P. Venner, Mamta Garg, Michael Kauffman, Dinesh Kumar Sinha, P. Moreau, Michele Cavo, Sundar Jagannath, Richard S., Chari A., Delimpasi S., Simonova M., Spicka I., Pour L., Kriachok I., Dimopoulos M.A., Pylypenko H., Auner H.W., Leleu X., Usenko G., Hajek R., Benjamin R., Dolai T.K., Sinha D.K., Venner C.P., Garg M., Stevens D.A., Quach H., Jagannath S., Moreau P., Levy M., Badros A., Anderson L.D., Bahlis N.J., Facon T., Mateos M.V., Cavo M., Chang H., Landesman Y., Chai Y., Arazy M., Shah J., Shacham S., Kauffman M.G., Grosicki S., and Richardson P.G.

Subjects
Adult, Male, medicine.medical_specialty, Population, Antineoplastic Agents, Gastroenterology, Dexamethasone, Antineoplastic Agent, Bortezomib, Young Adult, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Hydrazine, Humans, Progression-free survival, Young adult, education, Multiple myeloma, Research Articles, Aged, education.field_of_study, Hematology, Antineoplastic Combined Chemotherapy Protocol, business.industry, Cytogenetic Analysi, Triazoles, Middle Aged, medicine.disease, Progression-Free Survival, Peripheral neuropathy, Hydrazines, Treatment Outcome, Cytogenetic Analysis, Female, Triazole, business, Multiple Myeloma, medicine.drug, Research Article, Human
Abstract

In the phase 3 BOSTON study, patients with multiple myeloma (MM) after 1–3 prior regimens were randomized to once-weekly selinexor (an oral inhibitor of exportin 1 [XPO1]) plus bortezomib-dexamethasone (XVd) or twice-weekly bortezomib-dexamethasone (Vd). Compared with Vd, XVd was associated with significant improvements in median progression-free survival (PFS), overall response rate (ORR), and lower rates of peripheral neuropathy, with trends in overall survival (OS) favoring XVd. In BOSTON, 141 (35.1%) patients had MM with high-risk (presence of del[17p], t[4;14], t[14;16], or ≥4 copies of amp1q21) cytogenetics (XVd, n=70; Vd, n=71), and 261 (64.9%) exhibited standard-risk cytogenetics (XVd, n=125; Vd, n=136). Among patients with high-risk MM, median PFS was 12.91 months for XVd and 8.61 months for Vd (HR, 0.73 [95% CI, (0.4673, 1.1406)], p=0.082), and ORRs were 78.6% and 57.7%, respectively (OR 2.68; p= 0.004). In the standard-risk subgroup, median PFS was 16.62 months for XVd and 9.46 months for Vd (HR 0.61; p=0.004), and ORRs were 75.2% and 64.7%, respectively (OR 1.65; p=0.033). The safety profiles of XVd and Vd in both subgroups were consistent with the overall population. These data suggest that selinexor can confer benefits to patients with MM regardless of cytogenetic risk. ClinicalTrials.gov identifier: NCT03110562.

Published
2021

45. FoxO-1 contributes to the efficacy of the combination of the XPO1 inhibitor selinexor and cisplatin in ovarian carcinoma preclinical models

Author

Yosef Landesman, Nives Carenini, Lucia Minoli, Michelandrea De Cesare, Nadia Zaffaroni, Simone Stucchi, Paola Perego, Eugenio Scanziani, Serena Stamatakos, Christian Argueta, Emilio Ciusani, Cristina Corno, Laura Gatti, Corno, C, Stucchi, S, De Cesare, M, Carenini, N, Stamatakos, S, Ciusani, E, Minoli, L, Scanziani, E, Argueta, C, Landesman, Y, Zaffaroni, N, Gatti, L, and Perego, P

Subjects
0301 basic medicine, XPO1/CRM1 inhibitor, Drug Evaluation, Preclinical, Receptors, Cytoplasmic and Nuclear, Apoptosis, Pharmacology, Biochemistry, Mice, 0302 clinical medicine, RNA interference, Ovarian carcinoma, Antineoplastic Combined Chemotherapy Protocols, Hydrazine, Ovarian Neoplasms, Forkhead Box Protein O1, Blot, Hydrazines, Treatment Outcome, 030220 oncology & carcinogenesis, Female, Karyopherin, Human, medicine.drug, Mice, Nude, Karyopherins, Biology, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, Gene silencing, Cisplatin, Antineoplastic Combined Chemotherapy Protocol, Dose-Response Relationship, Drug, Animal, Ovarian Neoplasm, Apoptosi, Triazoles, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, Cell culture, Cancer research, Triazole, Ovarian cancer
Abstract

The XPO1/CRM1 inhibitor selinexor (KPT-330), is currently being evaluated in multiple clinical trials as an anticancer agent. XPO1 participates in the nuclear export of FoxO-1, which we previously found to be decreased in platinum-resistant ovarian carcinoma. The aim of this study was to determine whether enriching FoxO-1 nuclear localization using selinexor would increase ovarian cancer cell sensitivity to cisplatin. Selinexor, as a single agent, displayed a striking antiproliferative effect in different ovarian carcinoma cell lines. A schedule-dependent synergistic effect of selinexor in combination with cisplatin was found in cisplatin-sensitive IGROV-1, the combination efficacy being more evident in sensitive than in the resistant cells. In IGROV-1 cells, the combination was more effective when selinexor followed cisplatin exposure. A modulation of proteins involved in apoptosis (p53, Bax) and in cell cycle progression (p21WAF1) was found by Western blotting. Selinexor-treated cells exhibited enriched FoxO-1 nuclear staining. Knock-down experiments with RNA interference indicated that FOXO1-silenced cells displayed a reduced sensitivity to selinexor. FOXO1 silencing also tended to reduce the efficacy of the drug combination at selected cisplatin concentrations. Selinexor significantly inhibited tumor growth, induced FoxO-1 nuclear localization and improved the efficacy of cisplatin in IGROV-1 xenografts. Taken together, our results support FoxO-1 as one of the key factors promoting sensitivity towards selinexor and the synergistic interaction between cisplatin and selinexor in ovarian carcinoma cells with selected molecular backgrounds, highlighting the need for treatment regimens tailored to the molecular tumor features.

Published
2018
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46. The Functional Transcriptomic Landscape Informs Therapeutic Strategies in Multiple Myeloma.

Author

Sudalagunta PR, Canevarolo RR, Meads MB, Silva M, Zhao X, Cubitt CL, Sansil SS, DeAvila G, Alugubelli RR, Bishop RT, Tungesvik A, Zhang Q, Hampton O, Teer JK, Welsh EA, Yoder SJ, Shah BD, Hazlehurst L, Gatenby RA, Van Domelen DR, Chai Y, Wang F, DeCastro A, Bloomer AM, Siegel EM, Lynch CC, Sullivan DM, Alsina M, Nishihori T, Brayer J, Cleveland JL, Dalton W, Walker CJ, Landesman Y, Baz R, Silva AS, and Shain KH

Abstract

Several therapeutic agents have been approved for treating multiple myeloma (MM), a cancer of bone marrow resident plasma cells. Predictive biomarkers for drug response could help guide clinical strategies to optimize outcomes. Here, we present an integrated functional genomic analysis of tumor samples from MM patients that were assessed for their ex vivo drug sensitivity to 37 drugs, clinical variables, cytogenetics, mutational profiles, and transcriptomes. This analysis revealed a MM transcriptomic topology that generates "footprints" in association with ex vivo drug sensitivity that have both predictive and mechanistic applications. Validation of the transcriptomic footprints for the anti-CD38 monoclonal antibody daratumumab and the nuclear export inhibitor selinexor demonstrated that these footprints can accurately classify clinical responses. The analysis further revealed that daratumumab and selinexor have anti-correlated mechanisms of resistance, and treatment with a selinexor-based regimen immediately after a daratumumab-containing regimen was associated with improved survival in three independent clinical trials, supporting an evolutionary-based strategy involving sequential therapy. These findings suggest that this unique repository and computational framework can be leveraged to inform underlying biology and to identify therapeutic strategies to improve treatment of MM.

Published
2024
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47. Allosteric degraders induce CRL5 ASB8 mediated degradation of XPO1.

Author

Hudman-Wing CE, Fung HYJ, Cagatay T, Kwanten B, Niesman AB, Gharghabi M, Permentier B, Shakya B, Shacham S, Landesman Y, Lapalombella R, Daelemans D, and Chook YM

Abstract

The nuclear export receptor Exportin 1 (XPO1/CRM1) is often overexpressed in cancer cells resulting in aberrant localization of many cancer-related protein cargoes. The XPO1 inhibitor and cancer drug selinexor (KPT-330), and its analog KPT-185, block XPO1-cargo binding thereby restoring cargo localization. Selinexor binding induces cullin-RING E3 ubiquitin ligase (CRL) substrate receptor ASB8-mediated XPO1 degradation. Here we reveal the mechanism of inhibitor-XPO1 engagement by CRL5ASB8. Cryogenic electron microscopy (cryo-EM) structures show ASB8 binding to a large surface of selinexor/KPT-185-XPO1 that includes a three-dimensional degron unique to the drug-bound exportin. The structure explains weak XPO1-ASB8 binding in the absence of selinexor/KPT-185 that is unproductive for proteasomal degradation, and the substantial affinity increase upon selinexor/KPT-185 conjugation, which results in CRL5 ASB8 -mediated XPO1 ubiquitination. In contrast to previously characterized small molecule degraders, which all act as molecular glues, selinexor/KPT-185 binds extensively to XPO1 but hardly contacts ASB8. Instead, selinexor/KPT-185 binds XPO1 and stabilizes a unique conformation of the NES/inhibitor-binding groove that binds ASB8. Selinexor/KPT-185 is an allosteric degrader. We have explained how drug-induced protein degradation is mediated by a CRL5 system through an allosteric rather than a molecular glue mechanism, expanding the modes of targeted protein degradation beyond the well-known molecular glues of CRL4.

Published
2024
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48. Exportin 1 governs the immunosuppressive functions of myeloid-derived suppressor cells in tumors through ERK1/2 nuclear export.

Author

Daneshmandi S, Yan Q, Choi JE, Katsuta E, MacDonald CR, Goruganthu M, Roberts N, Repasky EA, Singh PK, Attwood K, Wang J, Landesman Y, McCarthy PL, and Mohammadpour H

Subjects
Animals, Humans, Mice, Cell Differentiation, Cell Line, Tumor, Cell Nucleus metabolism, Immune Tolerance, Interleukin-6 metabolism, MAP Kinase Signaling System, Mice, Inbred C57BL, Neoplasms immunology, Neoplasms pathology, STAT3 Transcription Factor metabolism, Active Transport, Cell Nucleus, Exportin 1 Protein, Karyopherins metabolism, Myeloid-Derived Suppressor Cells immunology, Myeloid-Derived Suppressor Cells metabolism, Receptors, Cytoplasmic and Nuclear metabolism
Abstract

Myeloid-derived suppressor cells (MDSCs) are a main driver of immunosuppression in tumors. Understanding the mechanisms that determine the development and immunosuppressive function of these cells could provide new therapeutic targets to improve antitumor immunity. Here, using preclinical murine models, we discovered that exportin 1 (XPO1) expression is upregulated in tumor MDSCs and that this upregulation is induced by IL-6-induced STAT3 activation during MDSC differentiation. XPO1 blockade transforms MDSCs into T-cell-activating neutrophil-like cells, enhancing the antitumor immune response and restraining tumor growth. Mechanistically, XPO1 inhibition leads to the nuclear entrapment of ERK1/2, resulting in the prevention of ERK1/2 phosphorylation following the IL-6-mediated activation of the MAPK signaling pathway. Similarly, XPO1 blockade in human MDSCs induces the formation of neutrophil-like cells with immunostimulatory functions. Therefore, our findings revealed a critical role for XPO1 in MDSC differentiation and suppressive functions; exploiting these new discoveries revealed new targets for reprogramming immunosuppressive MDSCs to improve cancer therapeutic responses., (© 2024. The Author(s), under exclusive licence to CSI and USTC.)

Published
2024
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49. ASPSCR1::TFE3 Drives Alveolar Soft Part Sarcoma by Inducing Targetable Transcriptional Programs.

Author

Sicinska E, Kola VSR, Kerfoot JA, Taddei ML, Al-Ibraheemi A, Hsieh YH, Church AJ, Landesman-Bollag E, Landesman Y, and Hemming ML

Subjects
Humans, Animals, Mice, Gene Expression Regulation, Neoplastic, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Cell Line, Tumor, Xenograft Model Antitumor Assays, Cyclin-Dependent Kinase 4 genetics, Cyclin-Dependent Kinase 4 metabolism, Cyclin-Dependent Kinase 4 antagonists & inhibitors, Female, Neovascularization, Pathologic genetics, Neovascularization, Pathologic pathology, Neovascularization, Pathologic metabolism, Intracellular Signaling Peptides and Proteins, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors metabolism, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors genetics, Sarcoma, Alveolar Soft Part genetics, Sarcoma, Alveolar Soft Part pathology, Sarcoma, Alveolar Soft Part metabolism, Cell Proliferation genetics, Oncogene Proteins, Fusion genetics, Oncogene Proteins, Fusion metabolism
Abstract

Alveolar soft part sarcoma (ASPS) is a rare mesenchymal malignancy driven by the ASPSCR1::TFE3 fusion. A better understanding of the mechanisms by which this oncogenic transcriptional regulator drives cancer growth is needed to help identify potential therapeutic targets. In this study, we characterized the transcriptional and chromatin landscapes of ASPS tumors and preclinical models, identifying the essential role of ASPSCR1::TFE3 in tumor cell viability by regulating core transcriptional programs involved in cell proliferation, angiogenesis, and mitochondrial biology. ASPSCR1::TFE3 directly interacted with key epigenetic regulators at enhancers and promoters to support ASPS-associated transcription. Among the effector programs driven by ASPSCR1::TFE3, cell proliferation was driven by high levels of cyclin D1 expression. Disruption of cyclin D1/CDK4 signaling led to a loss of ASPS proliferative capacity, and combined inhibition of CDK4/6 and angiogenesis halted tumor growth in xenografts. These results define the ASPS oncogenic program, reveal mechanisms by which ASPSCR1::TFE3 controls tumor biology, and identify a strategy for therapeutically targeting tumor cell-intrinsic vulnerabilities. Significance: The ASPSCR1::TFE3 fusion propels the growth of alveolar soft part sarcoma  by activating transcriptional programs that regulate proliferation, angiogenesis, mitochondrial biogenesis, and differentiation and can be therapeutically targeted to improve treatment., (©2024 American Association for Cancer Research.)

Published
2024
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50. Molecular analysis of XPO1 inhibitor and gemcitabine-nab-paclitaxel combination in KPC pancreatic cancer mouse model.

Author

Uddin MH, Al-Hallak MN, Khan HY, Aboukameel A, Li Y, Bannoura SF, Dyson G, Kim S, Mzannar Y, Azar I, Odisho T, Mohamed A, Landesman Y, Kim S, Beydoun R, Mohammad RM, Philip PA, Shields AF, and Azmi AS

Subjects
Animals, Mice, Disease Models, Animal, Gemcitabine administration & dosage, Paclitaxel administration & dosage, Hydrazines administration & dosage, Triazoles administration & dosage, Tumor Microenvironment, Single-Cell Gene Expression Analysis, Humans, Pancreatic Neoplasms drug therapy, Carcinoma, Pancreatic Ductal drug therapy, Exportin 1 Protein antagonists & inhibitors, Drug Combinations
Abstract

Background: The majority of pancreatic ductal adenocarcinoma (PDAC) patients experience disease progression while on treatment with gemcitabine and nanoparticle albumin-bound (nab)-paclitaxel (GemPac) necessitating the need for a more effective treatment strategy for this refractory disease. Previously, we have demonstrated that nuclear exporter protein exportin 1 (XPO1) is a valid therapeutic target in PDAC, and the selective inhibitor of nuclear export selinexor (Sel) synergistically enhances the efficacy of GemPac in pancreatic cancer cells, spheroids and patient-derived tumours, and had promising activity in a phase I study., Methods: Here, we investigated the impact of selinexor-gemcitabine-nab-paclitaxel (Sel-GemPac) combination on LSL-Kras G12D/+ ; LSL-Trp53 R172H/+ ; Pdx1-Cre (KPC) mouse model utilising digital spatial profiling (DSP) and single nuclear RNA sequencing (snRNAseq)., Results: Sel-GemPac synergistically inhibited the growth of the KPC tumour-derived cell line. The Sel-GemPac combination reduced the 2D colony formation and 3D spheroid formation. In the KPC mouse model, at a sub-maximum tolerated dose (sub-MTD) , Sel-GemPac enhanced the survival of treated mice compared to controls (p < .05). Immunohistochemical analysis of residual KPC tumours showed re-organisation of tumour stromal architecture, suppression of proliferation and nuclear retention of tumour suppressors, such as Forkhead Box O3a (FOXO3a). DSP revealed the downregulation of tumour promoting genes such as chitinase-like protein 3 (CHIL3/CHI3L3/YM1) and multiple pathways including phosphatidylinositol 3'-kinase-Akt (PI3K-AKT) signalling. The snRNAseq demonstrated a significant loss of cellular clusters in the Sel-GemPac-treated mice tumours including the CD44+ stem cell population., Conclusion: Taken together, these results demonstrate that the Sel-GemPac treatment caused broad perturbation of PDAC-supporting signalling networks in the KPC mouse model., Highlights: The majority of pancreatic ductal adenocarcinoma (PDAC) patients experience disease progression while on treatment with gemcitabine and nanoparticle albumin-bound (nab)-paclitaxel (GemPac). Exporter protein exportin 1 (XPO1) inhibitor selinexor (Sel) with GemPac synergistically inhibited the growth of LSL-KrasG12D/+; LSL-Trp53R172H/+; Pdx1-Cre (KPC) mouse derived cell line and enhanced the survival of mice. Digital spatial profiling shows that Sel-GemPac causes broad perturbation of PDAC-supporting signalling in the KPC model., (© 2023 The Authors. Clinical and Translational Medicine published by John Wiley & Sons Australia, Ltd on behalf of Shanghai Institute of Clinical Bioinformatics.)

Published
2023
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