Your search keyword '"Pawan K. Shahi"' showing total 5 results

1. A mutation in transmembrane protein 135 impairs lipid metabolism in mouse eyecups

Author

Michael Landowski, Vijesh J. Bhute, Tetsuya Takimoto, Samuel Grindel, Pawan K. Shahi, Bikash R. Pattnaik, Sakae Ikeda, and Akihiro Ikeda

Subjects

Medicine, Science

Abstract

Abstract Aging is a significant factor in the development of age-related diseases but how aging disrupts cellular homeostasis to cause age-related retinal disease is unknown. Here, we further our studies on transmembrane protein 135 (Tmem135), a gene involved in retinal aging, by examining the transcriptomic profiles of wild-type, heterozygous and homozygous Tmem135 mutant posterior eyecup samples through RNA sequencing (RNA-Seq). We found significant gene expression changes in both heterozygous and homozygous Tmem135 mutant mouse eyecups that correlate with visual function deficits. Further analysis revealed that expression of many genes involved in lipid metabolism are changed due to the Tmem135 mutation. Consistent with these changes, we found increased lipid accumulation in mutant Tmem135 eyecup samples. Since mutant Tmem135 mice have similar ocular pathologies as human age-related macular degeneration (AMD) eyes, we compared our homozygous Tmem135 mutant eyecup RNA-Seq dataset with transcriptomic datasets of human AMD donor eyes. We found similar changes in genes involved in lipid metabolism between the homozygous Tmem135 mutant eyecups and AMD donor eyes. Our study suggests that the Tmem135 mutation affects lipid metabolism as similarly observed in human AMD eyes, thus Tmem135 mutant mice can serve as a good model for the role of dysregulated lipid metabolism in AMD.

Published

2022

2. Hypoxic–ischemic injury causes functional and structural neurovascular degeneration in the juvenile mouse retina

Author

Ismail S. Zaitoun, Pawan K. Shahi, Andrew Suscha, Kore Chan, Gillian J. McLellan, Bikash R. Pattnaik, Christine M. Sorenson, and Nader Sheibani

Subjects

Medicine, Science

Abstract

Abstract Ischemic stroke is a major cause of long-term disabilities, including vision loss. Neuronal and blood vessel maturation can affect the susceptibility of and outcome after ischemic stroke. Although we recently reported that exposure of neonatal mice to hypoxia–ischemia (HI) severely compromises the integrity of the retinal neurovasculature, it is not known whether juvenile mice are similarly impacted. Here we examined the effect of HI injury in juvenile mice on retinal structure and function, in particular the susceptibility of retinal neurons and blood vessels to HI damage. Our studies demonstrated that the retina suffered from functional and structural injuries, including reduced b-wave, thinning of the inner retinal layers, macroglial remodeling, and deterioration of the vasculature. The degeneration of the retinal vasculature associated with HI resulted in a significant decrease in the numbers of pericytes and endothelial cells as well as an increase in capillary loss. Taken together, these findings suggest a need for juveniles suffering from ischemic stroke to be monitored for changes in retinal functional and structural integrity. Thus, there is an emergent need for developing therapeutic approaches to prevent and reverse retinal neurovascular dysfunction with exposure to ischemic stroke.

Published

2021

3. A mutation in transmembrane protein 135 impairs lipid metabolism in mouse eyecups

Author

Michael Landowski, Vijesh J. Bhute, Tetsuya Takimoto, Samuel Grindel, Pawan K. Shahi, Bikash R. Pattnaik, Sakae Ikeda, and Akihiro Ikeda

Subjects

Cell biology, Multidisciplinary, genetic structures, Molecular biology, Science, Membrane Proteins, Eye, Lipid Metabolism, eye diseases, Mice, Mutant Strains, Article, Mitochondrial Proteins, Disease Models, Animal, Macular Degeneration, Mutation, Genetics, Medicine, Animals, Humans, sense organs

Abstract

Aging is a significant factor in the development of age-related diseases but how aging disrupts cellular homeostasis to cause age-related retinal disease is unknown. Here, we further our studies on transmembrane protein 135 (Tmem135), a gene involved in retinal aging, by examining the transcriptomic profiles of wild-type, heterozygous and homozygous Tmem135 mutant posterior eyecup samples through RNA sequencing (RNA-Seq). We found significant gene expression changes in both heterozygous and homozygous Tmem135 mutant mouse eyecups that correlate with visual function deficits. Further analysis revealed that expression of many genes involved in lipid metabolism are changed due to the Tmem135 mutation. Consistent with these changes, we found increased lipid accumulation in mutant Tmem135 eyecup samples. Since mutant Tmem135 mice have similar ocular pathologies as human age-related macular degeneration (AMD) eyes, we compared our homozygous Tmem135 mutant eyecup RNA-Seq dataset with transcriptomic datasets of human AMD donor eyes. We found similar changes in genes involved in lipid metabolism between the homozygous Tmem135 mutant eyecups and AMD donor eyes. Our study suggests that the Tmem135 mutation affects lipid metabolism as similarly observed in human AMD eyes, thus Tmem135 mutant mice can serve as a good model for the role of dysregulated lipid metabolism in AMD.

Published

2021

4. Hypoxic-ischemic injury causes functional and structural neurovascular degeneration in the juvenile mouse retina

Author

Andrew Suscha, Gillian J. McLellan, Christine M. Sorenson, Bikash R. Pattnaik, Pawan K Shahi, Nader Sheibani, Ismail Zaitoun, and Kore Chan

Subjects

Pathology, medicine.medical_specialty, Cell biology, Molecular biology, Science, Degeneration (medical), 030204 cardiovascular system & hematology, Retina, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Ischemia, Developmental biology, medicine, Juvenile, Animals, Hypoxia, Ischemic Stroke, Hypoxic ischemic, Multidisciplinary, business.industry, Endothelial Cells, Retinal Vessels, Retinal, Neurovascular bundle, Capillaries, Disease Models, Animal, medicine.anatomical_structure, chemistry, Mouse Retina, Blood vessel maturation, Medicine, business, Pericytes, 030217 neurology & neurosurgery, Retinal Neurons, Neuroscience

Abstract

Ischemic stroke is a major cause of long-term disabilities, including vision loss. Neuronal and blood vessel maturation can affect the susceptibility of and outcome after ischemic stroke. Although we recently reported that exposure of neonatal mice to hypoxia–ischemia (HI) severely compromises the integrity of the retinal neurovasculature, it is not known whether juvenile mice are similarly impacted. Here we examined the effect of HI injury in juvenile mice on retinal structure and function, in particular the susceptibility of retinal neurons and blood vessels to HI damage. Our studies demonstrated that the retina suffered from functional and structural injuries, including reduced b-wave, thinning of the inner retinal layers, macroglial remodeling, and deterioration of the vasculature. The degeneration of the retinal vasculature associated with HI resulted in a significant decrease in the numbers of pericytes and endothelial cells as well as an increase in capillary loss. Taken together, these findings suggest a need for juveniles suffering from ischemic stroke to be monitored for changes in retinal functional and structural integrity. Thus, there is an emergent need for developing therapeutic approaches to prevent and reverse retinal neurovascular dysfunction with exposure to ischemic stroke.

Published

2020

5. Abnormal Electroretinogram after Kir7.1 Channel Suppression Suggests Role in Retinal Electrophysiology

Author

Bryce Aul, De-Ann M. Pillers, Andrea Moyer, Pawan K Shahi, Bikash R. Pattnaik, Akshita Pattnaik, Xinling Liu, and Jerod S. Denton

Subjects

Male, 0301 basic medicine, genetic structures, Abnormal electroretinogram, Fluorescent Antibody Technique, Gene Expression, lcsh:Medicine, CHO Cells, Biology, Models, Biological, Retina, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, Cricetulus, Electroretinography, medicine, Animals, Potassium Channels, Inwardly Rectifying, RNA, Small Interfering, lcsh:Science, Multidisciplinary, Retinal pigment epithelium, lcsh:R, Depolarization, Retinal, Anatomy, Hyperpolarization (biology), Immunohistochemistry, Photoreceptor outer segment, eye diseases, Cell biology, 030104 developmental biology, medicine.anatomical_structure, chemistry, Female, lcsh:Q, sense organs, Ion Channel Gating, Erg, Tomography, Optical Coherence, Photoreceptor Cells, Vertebrate

Abstract

The KCNJ13 gene encodes the inwardly rectifying potassium channel, Kir7.1. Mutations in this gene cause childhood blindness, in which the a- and b-wave responses of electroretinogram (ERG) are abolished. The ERG a-wave is the light-induced hyperpolarization of retinal photoreceptors, and the b-wave is the depolarization of ON-bipolar cells. The Kir7.1 channel is localized to the apical aspects of retinal pigment epithelium (RPE) cells and contributes to a delayed c-wave response. We sought to understand why a defect in an RPE ion-channel result in abnormal electrophysiology at the level of the retinal neurons. We have established the expression of Kir7.1 channels in the mouse RPE. ERGs recorded after mice Kir7.1 suppression by shRNA, or by blocking with VU590, showed reduced a-, b- and c-wave amplitudes. In contrast, the Kir7.1 blocker had no effect on the ex-vivo isolated mouse retina ERG where the RPE is not attached to the isolated retina preparation. Finally, we confirmed the specificity of VU590 action by inhibition of native mouse RPE Kir7.1 current in patch-clamp experiment. We propose that mutant RPE Kir7.1 channels contribute directly to the abnormal ERG associated with blindness via alterations in sub-retinal space K+ homeostasis in the vicinity of the photoreceptor outer segment.

Published

2017