Your search keyword '"Arya, Richa"' showing total 5 results

1. Cell death in development: Signaling pathways and core mechanisms.

Author

Arya R and White K

Subjects

Animals, Apoptosis, Humans, Neoplasms pathology, Neurodegenerative Diseases pathology, Cell Death, Drosophila cytology, Drosophila growth & development, Morphogenesis, Signal Transduction

Abstract

Programmed cell death eliminates unneeded and dangerous cells in a timely and effective manner during development. In this review, we examine the role cell death plays during development in worms, flies and mammals. We discuss signaling pathways that regulate developmental cell death, and describe how they communicate with the core cell death pathways. In most organisms, the majority of developmental cell death is seen in the nervous system. Therefore we focus on what is known about the regulation of developmental cell death in this tissue. Understanding how the cell death is regulated during development may provide insight into how this process can be manipulated in the treatment of disease., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

2. Hsp60D Is Essential for Caspase-Mediated Induced Apoptosis in Drosophila melanogaster

Author

Arya, Richa and Lakhotia, S. C.

Published

2008

3. A Cut/cohesin axis alters the chromatin landscape to facilitate neuroblast death.

Author

Arya, Richa, Gyonjyan, Seda, Harding, Katherine, Sarkissian, Tatevik, Ying Li, Lei Zhou, and White, Kristin

Subjects

*DNA-binding proteins, *NEURAL stem cells, *CELL death, *NERVOUS system

Abstract

Precise control of cell death in the nervous system is essential for development. Spatial and temporal factors activate the death of Drosophila neural stem cells (neuroblasts) by controlling the transcription of multiple cell death genes through a shared enhancer. The activity of this enhancer is controlled by abdominal A and Notch, but additional inputs are needed for proper specificity. Here, we show that the Cut DNA binding protein is required for neuroblast death, regulating reaper and grim downstream of the shared enhancer and of abdominal A expression. The loss of cut accelerates the temporal progression of neuroblasts from a state of low overall levels of H3K27me3 to a higher H3K27me3 state. This is reflected in an increase in H3K27me3 modifications in the cell death gene locus in the CNS on Cut knockdown. We also show that cut regulates the expression of the cohesin subunit Stromalin. Stromalin and the cohesin regulatory subunit Nipped-B are required for neuroblast death, and knockdown of Stromalin increases H3K27me3 levels in neuroblasts. Thus, Cut and cohesin regulate apoptosis in the developing nervous system by altering the chromatin landscape. [ABSTRACT FROM AUTHOR]

Published

2019

4. Cell death regulates muscle fiber number.

Author

Sarkissian, Tatevik, Arya, Richa, Gyonjyan, Seda, Taylor, Barbara, and White, Kristin

Subjects

*CELL death, *STEM cells, *NEURONS, *CENTRAL nervous system, *MUSCLE growth, *PHENOTYPES

Abstract

Cell death can have both cell autonomous and non-autonomous roles in normal development. Previous studies have shown that the central cell death regulators grim and reaper are required for the developmentally important elimination of stem cells and neurons in the developing central nervous system (CNS). Here we show that cell death in the nervous system is also required for normal muscle development. In the absence of grim and reaper , there is an increase in the number of fibers in the ventral abdominal muscles in the Drosophila adult. This phenotype can be partially recapitulated by inhibition of cell death specifically in the CNS, indicating a non-autonomous role for neuronal death in limiting muscle fiber number. We also show that FGFs produced in the cell death defective nervous system are required for the increase in muscle fiber number. Cell death in the muscle lineage during pupal stages also plays a role in specifying fiber number. Our work suggests that FGFs from the CNS act as a survival signal for muscle founder cells. Thus, proper muscle fiber specification requires cell death in both the nervous system and in the developing muscle itself. [ABSTRACT FROM AUTHOR]

Published

2016

5. Heat shock genes -- integrating cell survival and death.

Author

Arya, Richa, Mallik, Moushami, and Lakhotia, Subhash C.

Subjects

*CELL death, *HEAT shock proteins, *APOPTOSIS, *MITOCHONDRIA, *DROSOPHILA melanogaster, *CYTOCHROME c, *DROSOPHILA, *NON-coding RNA

Abstract

Heat shock induced gene expression and other cellular responses help limit the damage caused by stress and thus facilitate cellular recovery. Cellular damage also triggers apoptotic cell death through several pathways. This paper briefly reviews interactions of the major heat shock proteins with components of the apoptotic pathways. Hsp90, which acts as a chaperone for unstable signal transducers to keep them poised for activation, interacts with RIP and Akt and promotes NF-κB mediated inhibition of apoptosis; in addition it also blocks some steps in the apoptotic pathways. Hsp70 is mostly anti-apoptotic and acts at several levels like inhibition of translocation of Bax into mitochondria, release of cytochrome c from mitochondria, formation of apoptosome and inhibition of activation of initiator caspases. Hsp70 also modulates JNK, NF-κB and Akt signaling pathways in the apoptotic cascade. In contrast, Hsp60 has both anti- and pro-apoptotic roles. Cytosolic Hsp60 prevents translocation of the pro-apoptotic protein Bax into mitochondria and thus promotes cell survival but it also promotes maturation of procaspase-3, essential for caspase mediated cell death. Our recent in vivo studies show that RNAi for the Hsp60D in Drosophila melanogaster prevents induced apoptosis. Hsp27 exerts its anti-apoptotic influence by inhibiting cytochrome c and TNF-mediated cell death. αβ crystallin suppresses caspase-8 and cytochrome c mediated activation of caspase-3. Studies in our laboratory also reveal that absence or reduced levels of the developmentally active as well as stress induced non-coding hsrω transcripts, which are known to sequester diverse hnRNPs and related nuclear RNA-binding proteins, block induced apoptosis in Drosophila. Modulation of the apoptotic pathways by Hsps reflects their roles as "weak links" between various "hubs" in cellular networks. On the other hand, non-coding RNAs, by virtue of their potential to bind with multiple proteins, can act as "hubs" in these networks. In view of the integrative nature of living systems, it is not surprising that stress-induced genes, generally believed to primarily function in cell survival pathways, inhibit or even promote cell death pathways at multiple levels to ensure homeostasis at cell and/or organism level. The heat shock genes obviously do much more than merely help cells survive stress. [ABSTRACT FROM AUTHOR]

Published

2007