Your search keyword '"NSC243928"' showing total 6 results

1. NSC243928 Treatment Induces Anti-Tumor Immune Response in Mouse Mammary Tumor Models.

Author

Selvanesan, Benson Chellakkan, de Mingo Pulido, Alvaro, Varghese, Sheelu, Rohila, Deepak, Hupalo, Daniel, Gusev, Yuriy, Contente, Sara, Wilkerson, Matthew D., Dalgard, Clifton L., and Upadhyay, Geeta

Subjects

*THERAPEUTIC use of antineoplastic agents, *ANIMAL experimentation, *CANCER patients, *RESEARCH funding, *T cells, *BREAST tumors, *MICE, *CELL death, *IMMUNOTHERAPY

Abstract

Simple Summary: This study used two different syngeneic mouse mammary tumor models to determine the effect of a small molecule NSC243928 on intra-tumoral immune cells. We observed that NSC243928 treatment reduced the tumor burden in vivo and altered the wide range of immune cell infiltration in both models. These results pave the path for further study of the role of NSC243928 in immuno-oncology drug development for triple-negative breast cancer. NSC243928 induces cell death in triple-negative breast cancer cells in a LY6K-dependent manner. NSC243928 has been reported as an anti-cancer agent in the NCI small molecule library. The molecular mechanism of NSC243928 as an anti-cancer agent in the treatment of tumor growth in the syngeneic mouse model has not been established. With the success of immunotherapies, novel anti-cancer drugs that may elicit an anti-tumor immune response are of high interest in the development of novel drugs to treat solid cancer. Thus, we focused on studying whether NSC243928 may elicit an anti-tumor immune response in the in vivo mammary tumor models of 4T1 and E0771. We observed that NSC243928 induced immunogenic cell death in 4T1 and E0771 cells. Furthermore, NSC243928 mounted an anti-tumor immune response by increasing immune cells such as patrolling monocytes, NKT cells, B1 cells, and decreasing PMN MDSCs in vivo. Further studies are required to understand the exact mechanism of NSC243928 action in inducing an anti-tumor immune response in vivo, which can be used to determine a molecular signature associated with NSC243928 efficacy. NSC243928 may be a good target for future immuno-oncology drug development for breast cancer. [ABSTRACT FROM AUTHOR]

Published

2023

2. NSC243928 Treatment Induces Anti-Tumor Immune Response in Mouse Mammary Tumor Models

Author

Benson Chellakkan Selvanesan, Alvaro de Mingo Pulido, Sheelu Varghese, Deepak Rohila, Daniel Hupalo, Yuriy Gusev, Sara Contente, Matthew D. Wilkerson, Clifton L. Dalgard, and Geeta Upadhyay

Subjects

Cancer Research, NKT cells, Oncology, mammary tumor model, B1 cells, NSC243928, 4T1, E0771, myeloid derived suppressor cells, LY6K

Abstract

NSC243928 induces cell death in triple-negative breast cancer cells in a LY6K-dependent manner. NSC243928 has been reported as an anti-cancer agent in the NCI small molecule library. The molecular mechanism of NSC243928 as an anti-cancer agent in the treatment of tumor growth in the syngeneic mouse model has not been established. With the success of immunotherapies, novel anti-cancer drugs that may elicit an anti-tumor immune response are of high interest in the development of novel drugs to treat solid cancer. Thus, we focused on studying whether NSC243928 may elicit an anti-tumor immune response in the in vivo mammary tumor models of 4T1 and E0771. We observed that NSC243928 induced immunogenic cell death in 4T1 and E0771 cells. Furthermore, NSC243928 mounted an anti-tumor immune response by increasing immune cells such as patrolling monocytes, NKT cells, B1 cells, and decreasing PMN MDSCs in vivo. Further studies are required to understand the exact mechanism of NSC243928 action in inducing an anti-tumor immune response in vivo, which can be used to determine a molecular signature associated with NSC243928 efficacy. NSC243928 may be a good target for future immuno-oncology drug development for breast cancer.

Published

2023

3. Lymphocyte antigen 6K signaling to aurora kinase promotes advancement of the cell cycle and the growth of cancer cells, which is inhibited by LY6K-NSC243928 interaction.

Author

Selvanesan, Benson Chellakkan, Varghese, Sheelu, Andrys-Olek, Justyna, Arriaza, Ricardo Hernandez, Prakash, Rahul, Tiwari, Purushottam Babu, Hupalo, Daniel, Gusev, Yuriy, Patel, Megha Nitin, Contente, Sara, Sanda, Miloslav, Uren, Aykut, Wilkerson, Matthew D., Dalgard, Clifton Lee, Shimizu, Linda S., Chruszcz, Maksymilian, Borowski, Tomasz, and Upadhyay, Geeta

Subjects

*CANCER cell growth, *AURORA kinases, *CELL cycle, *TRIPLE-negative breast cancer, *SMALL molecules

Abstract

Lymphocyte antigen 6K (LY6K) is a small GPI-linked protein that is normally expressed in testes. Increased expression of LY6K is significantly associated with poor survival outcomes in many solid cancers, including cancers of the breast, ovary, gastrointestinal tract, head and neck, brain, bladder, and lung. LY6K is required for ERK-AKT and TGF-β pathways in cancer cells and is required for in vivo tumor growth. In this report, we describe a novel role for LY6K in mitosis and cytokinesis through aurora B kinase and its substrate histone H3 signaling axis. Further, we describe the structural basis of the molecular interaction of small molecule NSC243928 with LY6K protein and the disruption of LY6K-aurora B signaling in cell cycle progression due to LY6K-NSC243928 interaction. Overall, disruption of LY6K function via NSC243928 led to failed cytokinesis, multinucleated cells, DNA damage, senescence, and apoptosis of cancer cells. LY6K is not required for vital organ function, thus inhibition of LY6K signaling is an ideal therapeutic approach for hard-to-treat cancers that lack targeted therapy such as triple-negative breast cancer. • Discovery of a unique function for LY6K in mitosis and cytokinesis via aurora B kinase signaling in cancer cells. • Structural underpinnings of the interaction between the inhibitor NSC243928 and the protein LY6K. • Mechanism of action of small molecule NSC243928 in LY6K signaling. • NSC243928 inhibits cell cycle, disrupts mitosis and cytokinesis resulting in DNA damage, senescence, and cancer cell death. [ABSTRACT FROM AUTHOR]

Published

2023

4. Development of fluorophore labeled or biotinylated anticancer small molecule NSC243928.

Author

Prakash, Rahul, Goodlett, Dustin W., Varghese, Sheelu, Andrys, Justyna, Gbadamosi, Fahidat A., Arriaza, Ricardo H., Patel, Megha, Tiwari, Purushottam B., Borowski, Tomasz, Chruszcz, Maksymilian, Shimizu, Linda S., and Upadhyay, Geeta

Subjects

*SMALL molecules, *TRIPLE-negative breast cancer, *STREPTAVIDIN, *SURFACE plasmon resonance, *MOLECULAR dynamics, *CANCER cells, *ALKYLATING agents

Abstract

[Display omitted] Small molecule NSC243928 binds with LY6K, a potential target for the treatment of triple-negative breast cancer, and induces cancer cell death with an unclear mechanism. We have developed chemical tools to identify the molecular mechanisms of NSC243928-LY6K interaction. Herein, we report on the development and synthesis of biotinylated and fluorophore-tethered derivatives of NSC243928 guided by docking studies and molecular dynamics. Surface plasmon resonance assay indicates that these derivatives retained a direct binding with LY6K protein. Confocal analysis revealed that nitrobenzoxadiazole (NBD) fluorophore tagged NSC243928 is retained in LY6K expressing cancer cells. These novel modified compounds will be employed in future in vitro and in vivo studies to understand the molecular mechanisms of NSC243928 mediated cancer cell death. These studies will pave the path for developing novel targeted therapeutics and understanding any potential side-effects of these treatments for hard-to-treat cancers such as triple-negative breast cancer or other cancers with high expression of LY6K. [ABSTRACT FROM AUTHOR]

Published

2023

5. Small Molecule Binds with Lymphocyte Antigen 6K to Induce Cancer Cell Death

Author

Aykut Üren, Senyi Benti, Linda S. Shimizu, Mark D. Smith, Dustin W. Goodlett, Grant B Kern, Maksymilian Chruszcz, Purushottam B. Tiwari, Geeta Upadhyay, and Leily Daneshian

Subjects

0301 basic medicine, Cancer Research, cervical cancer, Lymphocyte Antigen 6K, small molecule, lcsh:RC254-282, Article, ly6k, HeLa, 03 medical and health sciences, nsc243928, 0302 clinical medicine, Gene expression, medicine, biology, Chemistry, Head and neck cancer, Small Molecule Libraries, Cancer, medicine.disease, biology.organism_classification, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Small molecule, 3. Good health, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, surface plasmon resonance

Abstract

Elevated gene expression of Lymphocyte antigen 6K (LY6K) in cancer cells is associated with poor survival outcomes in multiple different cancer types including cervical, breast, ovarian, lung, and head and neck cancer. Since inhibition of LY6K expression inhibits cancer cell growth, we set out to explore whether pharmacological inhibition of LY6K could produce the same effect. We screened small molecule libraries for direct binding to recombinant LY6K protein in a surface plasmon resonance assay. We found that NSC243928 directly binds to the full-length and mature forms of LY6K and inhibits growth of HeLa cells that express LY6K. NSC243928 did not display binding with LY6D or LY6E. Our data demonstrate a first-time proof of principle study that pharmacological inhibition of LY6K using small molecules in cancer cells is a valid approach to developing targeted therapies against LY6K. This approach will be specifically relevant in hard-to-treat cancers where LY6K is highly expressed, such as cervical, pancreatic, ovarian, head and neck, lung, gastric, and triple-negative breast cancers.

Published

2020

6. Small Molecule Binds with Lymphocyte Antigen 6K to Induce Cancer Cell Death.

Author

Benti, Senyi, Tiwari, Purushottam B., Goodlett, Dustin W., Daneshian, Leily, Kern, Grant B., Smith, Mark D., Uren, Aykut, Chruszcz, Maksymilian, Shimizu, Linda S., and Upadhyay, Geeta

Subjects

*LYMPHOCYTE metabolism, *ANTIGENS, *ANTINEOPLASTIC agents, *CELL death, *CELL lines, *LYMPHOCYTES, *TUMORS, *SURFACE plasmon resonance, *TREATMENT effectiveness, *PHARMACODYNAMICS

Abstract

Elevated gene expression of Lymphocyte antigen 6K (LY6K) in cancer cells is associated with poor survival outcomes in multiple different cancer types including cervical, breast, ovarian, lung, and head and neck cancer. Since inhibition of LY6K expression inhibits cancer cell growth, we set out to explore whether pharmacological inhibition of LY6K could produce the same effect. We screened small molecule libraries for direct binding to recombinant LY6K protein in a surface plasmon resonance assay. We found that NSC243928 directly binds to the full-length and mature forms of LY6K and inhibits growth of HeLa cells that express LY6K. NSC243928 did not display binding with LY6D or LY6E. Our data demonstrate a first-time proof of principle study that pharmacological inhibition of LY6K using small molecules in cancer cells is a valid approach to developing targeted therapies against LY6K. This approach will be specifically relevant in hard-to-treat cancers where LY6K is highly expressed, such as cervical, pancreatic, ovarian, head and neck, lung, gastric, and triple-negative breast cancers. [ABSTRACT FROM AUTHOR]

Published

2020