Your search keyword '"Elavazhagan, Saranya"' showing total 2 results

1. Active hexose-correlated compound enhances extrinsic-pathway-mediated apoptosis of Acute Myeloid Leukemic cells.

Author

Fatehchand, Kavin, Santhanam, Ramasamy, Shen, Brenda, Erickson, Ericka L., Gautam, Shalini, Elavazhagan, Saranya, Mo, Xiaokui, Belay, Tesfaye, Tridandapani, Susheela, and Butchar, Jonathan P.

Subjects

ACUTE myeloid leukemia, CANCER cells, HEXOSES, ANTINEOPLASTIC agents, APOPTOSIS, DRUG activation, PATIENTS

Abstract

Active Hexose Correlated Compound (AHCC) has been shown to have many immunostimulatory and anti-cancer activities in mice and in humans. As a natural product, AHCC has potential to create safer adjuvant therapies in cancer patients. Acute Myeloid Leukemia (AML) is the least curable and second-most common leukemia in adults. AML is especially terminal to those over 60 years old, where median survival is only 5 to 10 months, due to inability to receive intensive chemotherapy. Hence, the purpose of this study was to investigate the effects of AHCC on AML cells both in vitro and in vivo. Results showed that AHCC induced Caspase-3-dependent apoptosis in AML cell lines as well as in primary AML leukopheresis samples. Additionally, AHCC induced Caspase-8 cleavage as well as Fas and TRAIL upregulation, suggesting involvement of the extrinsic apoptotic pathway. In contrast, monocytes from healthy donors showed suppressed Caspase-3 cleavage and lower cell death. When tested in a murine engraftment model of AML, AHCC led to significantly increased survival time and decreased blast counts. These results uncover a mechanism by which AHCC leads to AML-cell specific death, and also lend support for the further investigation of AHCC as a potential adjuvant for the treatment of AML. [ABSTRACT FROM AUTHOR]

Published

2017

2. Granzyme B Expression Is Enhanced in Human Monocytes by TLR8 Agonists and Contributes to Antibody-Dependent Cellular Cytotoxicity.

Author

Elavazhagan, Saranya, Fatehchand, Kavin, Santhanam, Vikram, Huiqing Fang, Li Ren, Gautam, Shalini, Reader, Brenda, Xiaokui Mo, Cheney, Carolyn, Briercheck, Edward, Vasilakos, John P., Dietsch, Gregory N., Hershberg, Robert M., Caligiuri, Michael, Byrd, John C., Butchar, Jonathan P., and Tridandapani, Susheela

Subjects

*CANCER treatment, *PROTEIN binding, *KILLER cells, *MONOCYTES, *PROTEOLYTIC enzymes

Abstract

FcγRs are critical mediators of mAb cancer therapies, because they drive cytotoxic processes upon binding of effector cells to opsonized targets. Along with NK cells, monocytes are also known to destroy Ab-coated targets via Ab-dependent cellular cytotoxicity (ADCC). However, the precise mechanisms by which monocytes carry out this function have remained elusive. In this article, we show that human monocytes produce the protease granzyme B upon both FcγR and TLR8 activation. Treatment with TLR8 agonists elicited granzyme B and also enhanced FcγR-mediated granzyme B production in an additive fashion. Furthermore, monocyte-mediated ADCC against cetuximab-coated tumor targets was enhanced by TLR8 agonist treatment, and this enhancement of ADCC required granzyme B. Hence we have identified granzyme B as an important mediator of FcγR function in human monocytes and have uncovered another mechanism by which TLR8 agonists may enhance FcγR-based therapies. [ABSTRACT FROM AUTHOR]

Published

2015