Your search keyword '"Shah, Mithun Vinod"' showing total 6 results

1. Therapeutic efficacy of FTY720 in a rat model of NK-cell leukemia.

Author

Liao A, Broeg K, Fox T, Tan SF, Watters R, Shah MV, Zhang LQ, Li Y, Ryland L, Yang J, Aliaga C, Dewey A, Rogers A, Loughran K, Hirsch L, Jarbadan NR, Baab KT, Liao J, Wang HG, Kester M, Desai D, Amin S, Loughran TP Jr, and Liu X

Subjects

Animals, Blotting, Western, Cell Proliferation drug effects, Chronic Disease, Fingolimod Hydrochloride, Humans, Killer Cells, Natural immunology, Killer Cells, Natural pathology, Leukemia immunology, Leukemia pathology, Male, Myeloid Cell Leukemia Sequence 1 Protein, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-bcl-2 metabolism, RNA, Small Interfering genetics, Rats, Rats, Inbred F344, Sphingosine therapeutic use, Apoptosis drug effects, Immunosuppressive Agents therapeutic use, Killer Cells, Natural drug effects, Leukemia drug therapy, Propylene Glycols therapeutic use, Sphingosine analogs & derivatives

Abstract

NK-cell leukemia is a clonal expansion of NK cells. The illness can occur in an aggressive or chronic form. We studied cell lines from human and rat NK-cell leukemias (aggressive NK-cell leukemia) as well as samples from patients with chronic NK-cell leukemia to investigate pathogenic mechanisms. Here we report that Mcl-1 was overexpressed in leukemic NK cells and that knockdown of Mcl-1 induced apoptosis in these leukemic cells. In vitro treatment of human and rat NK leukemia cells with FTY720 led to caspase-dependent apoptosis and decreased Mcl-1 expression in a time- and-dose-dependent manner. These biologic effects could be inhibited by blockade of reactive oxygen species generation and the lysosomal degradation pathway. Lipidomic analyses after FTY720 treatment demonstrated elevated levels of sphingosine, which mediated apoptosis of leukemic NK cells in vitro. Importantly, systemic administration of FTY720 induced complete remission in the syngeneic Fischer rat model of NK-cell leukemia. Therapeutic efficacy was associated with decreased expression of Mcl-1 in vivo. These data demonstrate that therapeutic benefit of FTY720 may result from both altered sphingolipid metabolism as well as enhanced degradation of a key component of survival signaling.

Published

2011

2. Network Model of Survival Signaling in Large Granular Lymphocyte Leukemia

Author

Zhang, Ranran, Shah, Mithun Vinod, Yang, Jun, Nyland, Susan B., Liu, Xin, Yun, Jong K., Albert, Réka, and Loughran,, Thomas P.

Published

2008

3. Network model of survival signaling in large granular lymphocyte leukemia.

Author

Ranran Zhang, Shah, Mithun Vinod, Jun Yang, Nyland, Susan B., Xin Liu, Yun, Jong K., AIbert, Réka, and Loughran Jr., Thomas P.

Subjects

*T cells, *LYMPHOCYTES, *LEUKEMIA, *ANTIGENS, *CANCER, *TUMORS, *VACCINES

Abstract

T cell large granular lymphocyte (T-LGL) leukemia features a clonal expansion of antigen-primed, competent, cytotoxic T lymphocytes (CTL). To systematically understand signaling components that determine the survival of CTL in T-LGL leukemia, we constructed a T-LGL survival signaling network by integrating the signaling pathways involved in normal CTL activation and the known deregulations of survival signaling in leukemic T-LGL. This network was subsequently translated into a predictive, discrete, dynamic model. Our model suggests that the persistence of IL-15 and PDGF is sufficient to reproduce all known deregulations in leukemic T-LGL. This finding leads to the following predictions: (`) Inhibiting PDGF signaling induces apoptosis in leukemic T-LGL. (ii) Sphingosine kinase 1 and NFκB are essential for the long-term survival of CTL in T-LGL leukemia. (iii) NFκB functions downstream of PI3K and prevents apoptosis through maintaining the expression of myeloid cell leukemia sequence 1. (iv) T box expressed in T cells (T-bet) should be constitutively activated concurrently with NFκB activation to reproduce the leukemic T-LGL phenotype. We validated these predictions experimentally. Our study provides a model describing the signaling network involved in maintaining the long-term survival of competent CTL in humans. The model will be useful in identifying potential therapeutic targets for T-LGL leukemia and generating long-term competent CTL necessary for tumor and cancer vaccine development. [ABSTRACT FROM AUTHOR]

Published

2008

4. Genetic and Genomic Landscape of Secondary and Therapy-Related Acute Myeloid Leukemia.

Author

Higgins, Alexandra and Shah, Mithun Vinod

Subjects

*ACUTE myeloid leukemia, *PATHOLOGY, *RNA splicing, *LEUKEMIA, *MYELODYSPLASTIC syndromes

Abstract

A subset of acute myeloid leukemia (AML) arises either from an antecedent myeloid malignancy (secondary AML, sAML) or as a complication of DNA-damaging therapy for other cancers (therapy-related myeloid neoplasm, t-MN). These secondary leukemias have unique biological and clinical features that distinguish them from de novo AML. Over the last decade, molecular techniques have unraveled the complex subclonal architecture of sAML and t-MN. In this review, we compare and contrast biological and clinical features of de novo AML with sAML and t-MN. We discuss the role of genetic mutations, including those involved in RNA splicing, epigenetic modification, tumor suppression, transcription regulation, and cell signaling, in the pathogenesis of secondary leukemia. We also discuss clonal hematopoiesis in otherwise healthy individuals, as well as in the context of another malignancy, and how it challenges the conventional notion of sAML/t-MN. We conclude by summarizing the current and emerging treatment strategies, including allogenic transplant, in these complex scenarios. [ABSTRACT FROM AUTHOR]

Published

2020

5. Therapeutic efficacy of FTY720 in a rat model of NK-cell leukemia.

Author

Aijun Liao, Broeg, Kathleen, Fox, Todd, Su-Fern Tan, Watters, Rebecca, Shah, Mithun Vinod, Zhang, Lucy Q., Yongping Li, Ryland, Lindsay, Jun Yang, Aliaga, Cesar, Dewey, Alden, Rogers, Andrew, Loughran, Kelly, Hirsch, Leah, Jarbadan, Nancy Ruth, Baab, Kendall Thomas, Liao, Jason, Hong-Gang Wang, and Kester, Mark

Subjects

*KILLER cells, *LEUKEMIA, *LABORATORY rats, *APOPTOSIS, *LYSOSOMAL storage diseases, *SPHINGOLIPIDS

Abstract

NK-cell leukemia is a clonal expansion of NK cells. The illness can occur in an aggressive or chronic form. We studied cell lines from human and rat NK-cell leukemias (aggressive NK-cell leukemia) as well as samples from patients with chronic NK-cell leukemia to investigate pathogenic mechanisms. Here we report that Mcl-1 was overexpressed in leukemic NK cells and that knockdown of Mcl-1 induced apoptosis in these leukemic cells. In vitro treatment of human and rat NK leukemia cells with FTY720 led to caspase-dependent apoptosis and decreased Mcl-1 expression in a time- and-dose-dependent manner. These biologic effects could be inhibited by blockade of reactive oxygen species generation and the lysosomal degradation pathway. Lipidomic analyses after FTY720 treatment demonstrated elevated levels of sphingosine, which mediated apoptosis of leukemic NK cells in vitro. Importantly, systemic administration of FTY720 induced complete remission in the syngeneic Fischer rat model of NK-cell leukemia. Therapeutic efficacy was associated with decreased expression of Mcl-1 in vivo. These data demonstrate that therapeutic benefit of FTY720 may result from both altered sphingolipid metabolism as well as enhanced degradation of a key component of survival signaling. [ABSTRACT FROM AUTHOR]

Published

2011

6. NKp46 identifies an NKT cell subset susceptible to leukemic transformation in mouse and human.

Author

Jianhua Yu, Mitsui, Takeki, Min Wei, Hsiaoyin Mao, Butchar, Jonathan P., Shah, Mithun Vinod, Jianying Zhang, Anjali Mishra, Alvarez-Breckenridge, Christopher, Xingluo Liu, Shujun Liu, Yokohama, Akihiko, Trotta, Rossana, Marcucci, Guido, Benson Jr., Don M., Loughran Jr., Thomas P., Tridandapani, Susheela, and Caligiuri, Michael A.

Subjects

*LYMPHOCYTE transformation, *LEUKEMIA, *DISEASE susceptibility, *TRANSGENIC mice, *GROWTH factors, *T cells, *PATIENTS

Abstract

IL-15 may have a role in the development of T cell large granular lymphocyte (T-LGL) or NKT leukemias. However, the mechanisms of action and the identity of the cell subset that undergoes leukemic transformation remain elusive. Here we show that in both mice and humans, NKp46 expression marks a minute population of WT NKT cells with higher activity and potency to become leukemic. Virtually 100% of T-LGL leukemias in IL-15 transgenic mice expressed NKp46, as did a majority of human T-LGL leukemias. The minute NKp46- NKT population, but not the NKp46 NKT population, was selectively expanded by overexpression of endogenous IL-15. Importantly, IL-15 transgenic NKp46 NKT cells did not become NKp46+ in vivo, suggesting that NKp46+ T-LGL leukemia cells were the malignant counterpart of the minute WT NKp4+ NKT population. Mechanistically, NKp46+ NKT cells possessed higher responsiveness to IL-is in vitro and in vivo compared with that of their NKp46- NKT counterparts. Furthermore, interruption of IL-15 signaling using a neutralizing antibody could prevent LGL leukemia in IL-15 transgenic mice. Collectively, our data demonstrate that NKp46 identifies a functionally distinct NKT subset in mice and humans that appears to be directly susceptible to leukemic transformation when IL-15 is overexpressed. Thus, IL-15 signaling and NKp46 may be useful targets in the treatment of patients with T-LGL or NKT leukemia. [ABSTRACT FROM AUTHOR]

Published

2011