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Dive into the research topics where R. Krishnamoorthy is active.

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Featured researches published by R. Krishnamoorthy.


Stem Cells | 2015

Continuous non-cell autonomous reprogramming to generate retinal ganglion cells for glaucomatous neuropathy.

Sowmya Parameswaran; Shashank M. Dravid; Pooja Teotia; R. Krishnamoorthy; Fang Qiu; Carol B. Toris; John C. Morrison; Iqbal Ahmad

Glaucoma, where the retinal ganglion cells (RGCs) carrying the visual signals from the retina to the visual centers in the brain are progressively lost, is the most common cause of irreversible blindness. The management approaches, whether surgical, pharmacological, or neuroprotective do not reverse the degenerative changes. The stem cell approach to replace dead RGCs is a viable option but currently faces several barriers, such as the lack of a renewable, safe, and ethical source of RGCs that are functional and could establish contacts with bona fide targets. To address these barriers, we have derived RGCs from the easily accessible adult limbal cells, reprogrammed to pluripotency by a non‐nucleic acid approach, thus circumventing the risk of insertional mutagenesis. The generation of RGCs from the induced pluripotent stem (iPS) cells, also accomplished non‐cell autonomously, recapitulated the developmental mechanism, ensuring the predictability and stability of the acquired phenotype, comparable to that of native RGCs at biochemical, molecular, and functional levels. More importantly, the induced RGCs expressed axonal guidance molecules and demonstrated the potential to establish contacts with specific targets. Furthermore, when transplanted in the rat model of ocular hypertension, these cells incorporated into the host RGC layer and expressed RGC‐specific markers. Transplantation of these cells in immune‐deficient mice did not produce tumors. Together, our results posit retinal progenitors generated from non‐nucleic acid‐derived iPS cells as a safe and robust source of RGCs for replacing dead RGCs in glaucoma. Stem Cells 2013;33:1743–1758


Investigative Ophthalmology & Visual Science | 2015

Overexpression of the POU Domain Transcription Factor Brn-3b leads to Upregulation of the Pro-survival Factor Bcl-2 in Rat Retinal Ganglion Cells

Nitasha R. Phatak; Dorota Stankowska; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2015

Endothelin-Mediated Gene Expression in Rat Retinal Ganglion Cells

Shaoqing He; Yong H Park; Thomas Yorio; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2014

Endothelin B (ETB) Receptors Contribute to Neurodegeneration in a Rodent Model of Glaucoma via Upregulation of c-Jun and Bax

Alena Z. Minton; Shaoqing He; Hai-Ying Ma; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2014

Endothelins’ effects on gene expression in rat retinal ganglion cells

Shaoqing He; Yong H Park; Thomas Yorio; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2014

OVEREXPRESSION OF THE POU DOMAIN TRANSCRIPTION FACTOR, BRN3B CAUSES NEURITE OUTGROWTH IN CULTURED PC 12 CELLS UNDER CONDITION OF OXYGEN GLUCOSE DEPRIVATION

Nitasha R. Phatak; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2013

AP-1 and C/EBPβ Regulate Endothelin B (ETB) Receptor in Retinas of Rats in Response to Elevated Intraocular Pressure

Shaoqing He; Alena Z. Minton; Hai-Ying Ma; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2012

Endothelin B Receptors Contribute to Neurodegeneration in a Rodent Model of Glaucoma

Alena Z. Minton; Nitasha R. Phatak; Hai-Ying Ma; Dorota Stankowska; Shaoqing He; Brett Mueller; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2012

Transcriptional Regulation of Endothelin B (ETB) Receptor in Retinas of Rats in Response to Elevated Intraocular Pressure

Shaoqing He; Alena Z. Minton; Dorota Stankowska; R. Krishnamoorthy


Investigative Ophthalmology & Visual Science | 2011

Neurodegenerative Effects of Endothelin B Receptors in a Rodent Model of Glaucoma

Alena Z. Minton; Nitasha R. Phatak; Brett Mueller; Hai-Ying Ma; Ming Jiang; Shaoqing He; R. Krishnamoorthy

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Thomas Yorio

University of North Texas

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Hai-Ying Ma

University of North Texas Health Science Center

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Shaoqing He

University of North Texas

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Alena Z. Minton

University of North Texas

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V. Rao

University of North Texas Health Science Center

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A. Dibas

University of North Texas

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Brett Mueller

University of North Texas

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Ming Jiang

University of North Texas

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