Your search keyword '"Dheer, Yogita"' showing total 3 results

1. Molecular determinants and interaction data of cyclic peptide inhibitor with the extracellular domain of TrkB receptor

Author

Chitranshi, Nitin, Gupta, Vivek, Dheer, Yogita, Gupta, Veer, Vander Wall, Roshana, Graham, Stuart, Chitranshi, Nitin, Gupta, Vivek, Dheer, Yogita, Gupta, Veer, Vander Wall, Roshana, and Graham, Stuart

Abstract

TrkB is a high affinity receptor for the brain derived neurotrophic factor (BDNF) and its phosphorylation stimulates activation of several intracellular signalling pathways linked to cellular growth, differentiation and maintenance. Identification of various activators and inhibitors of the TrkB receptor and greater understanding their binding mechanisms is critical to elucidate the biochemical and pharmacological pathways and analyse various protein crystallization studies. The data presented here is related to the research article entitled "Brain Derived neurotrophic factor is involved in the regulation of glycogen synthase kinase 3β (GSK3β) signalling" [1]. Cyclotraxin B (CTXB) is a disulphide bridge linked cyclic peptide molecule that interacts with TrkB receptor and inhibits the BDNF/TrkB downstream signalling. This article reports for the first time binding mechanism and interaction parameters of CTXB with the TrkB receptor. The molecular model of CTXB has been generated and it's docking with TrkB domain carried out to determine the critical residues involved in the protein peptide interaction. © 2016 The Authors.

Published

2016

2. Amyloid β accumulation and inner retinal degenerative changes in Alzheimer’s disease transgenic mouse

Author

Gupta, Vivek K., Chitranshi, Nitin, Gupta, Veer B., Golzan, Mojtaba, Dheer, Yogita, Wall, Roshana Vander, Georgevsky, Dana, King, Anna E., Vickers, James C., Chung, Roger, Graham, Stuart, Gupta, Vivek K., Chitranshi, Nitin, Gupta, Veer B., Golzan, Mojtaba, Dheer, Yogita, Wall, Roshana Vander, Georgevsky, Dana, King, Anna E., Vickers, James C., Chung, Roger, and Graham, Stuart

Abstract

The APP-PS1δE9 mouse model of Alzheimer's disease (AD) exhibits age dependent amyloid β (Aβ) plaque formation in their central nervous system due to high expression of mutated human APP and PSEN1 transgenes. Here we evaluated Aβ deposition and changes in soluble Aβ accumulation in the retinas of aged APP-PS1 mice using a combination of immunofluorescence, retinal flat mounts and western blotting techniques. Aβ accumulation in the retina has previously been shown to be associated with retinal ganglion cell apoptosis in animal models of glaucoma. This study investigated changes in the inner retinal function and structure in APP-PS1 mice using electrophysiology and histological approaches respectively. We report for the first time a significant decline in scotopic threshold response (STR) amplitudes which represents inner retinal function in transgenic animals compared to the wild type counterparts (p < 0.0001). Thinning of the retina particularly involving inner retinal layers and reduction in axonal density in the optic nerve was also observed. TUNEL staining was performed to examine neuronal apoptosis in the inner retina. Intraocular pressure (IOP) measurements showed that APP-PS1δE9 mice had a slightly elevated IOP, but the significance of this finding is not yet known. Together, these results substantiate previous observations and highlight that APP-PS1δE9 mice show evidence of molecular, functional and morphological degenerative changes in the inner retina.

Published

2016

3. One protein, multiple pathologies: multifaceted involvement of amyloid β in neurodegenerative disorders of the brain and retina

Author

Gupta, Vivek, Gupta, Veer, Chitranshi, Nitin, Gangoda, Sumudu, Vander Wall, Roshana, Abbasi, Mojdeh, Golzan, Mojtaba, Dheer, Yogita, Shah, Tejal, Avolio, Alberto, Chung, Roger, Martins, Ralph, Graham, Stuart, Gupta, Vivek, Gupta, Veer, Chitranshi, Nitin, Gangoda, Sumudu, Vander Wall, Roshana, Abbasi, Mojdeh, Golzan, Mojtaba, Dheer, Yogita, Shah, Tejal, Avolio, Alberto, Chung, Roger, Martins, Ralph, and Graham, Stuart

Abstract

Accumulation of amyloid β (Aβ) and its aggregates in the ageing central nervous system is regarded synonymous to Alzheimer’s disease (AD) pathology. Despite unquestionable advances in mechanistic and diagnostic aspects of the disease understanding, the primary cause of Aβ accumulation as well as its in vivo roles remains elusive; nonetheless, the majority of the efforts to address pathological mechanisms for therapeutic development are focused towards moderating Aβ accumulation in the brain. More recently, Aβ deposition has been identified in the eye and is linked with distinct age-related diseases including age-related macular degeneration, glaucoma as well as AD. Awareness of the Aβ accumulation in these markedly different degenerative disorders has led to an increasing body of work exploring overlapping mechanisms, a prospective biomarker role for Aβ and the potential to use retina as a model for brain related neurodegenerative disorders. Here, we present an integrated view of current understanding of the retinal Aβ deposition discussing the accumulation mechanisms, anticipated impacts and outlining ameliorative approaches that can be extrapolated to the retina for potential therapeutic benefits. Further longitudinal investigations in humans and animal models will determine retinal Aβ association as a potential pathognomonic, diagnostic or prognostic biomarker. © 2016 Springer International Publishing

Published

2016