Your search keyword '"Rajan K. C."' showing total 10 results

1. Zmiz1 is a novel regulator of brain development associated with autism and intellectual disability

Author

Rajan K. C., Alina S. Tiemroth, Abbigail N. Thurmon, Stryder M. Meadows, and Maria J. Galazo

Subjects

Zmiz1, de novo mutations, neurodevelopment, neurodevelopmental disorders, autism, Psychiatry, RC435-571

Abstract

Neurodevelopmental disorders (NDDs) are a class of pathologies arising from perturbations in brain circuit formation and maturation with complex etiological triggers often classified as environmental and genetic. Neuropsychiatric conditions such as autism spectrum disorders (ASD), intellectual disability (ID), and attention deficit hyperactivity disorders (ADHD) are common NDDs characterized by their hereditary underpinnings and inherent heterogeneity. Genetic risk factors for NDDs are increasingly being identified in non-coding regions and proteins bound to them, including transcriptional regulators and chromatin remodelers. Importantly, de novo mutations are emerging as important contributors to NDDs and neuropsychiatric disorders. Recently, de novo mutations in transcriptional co-factor Zmiz1 or its regulatory regions have been identified in unrelated patients with syndromic ID and ASD. However, the role of Zmiz1 in brain development is unknown. Here, using publicly available databases and a Zmiz1 mutant mouse model, we reveal that Zmiz1 is highly expressed during embryonic brain development in mice and humans, and though broadly expressed across the brain, Zmiz1 is enriched in areas prominently impacted in ID and ASD such as cortex, hippocampus, and cerebellum. We investigated the relationship between Zmiz1 structure and pathogenicity of protein variants, the epigenetic marks associated with Zmiz1 regulation, and protein interactions and signaling pathways regulated by Zmiz1. Our analysis reveals that Zmiz1 regulates multiple developmental processes, including neurogenesis, neuron connectivity, and synaptic signaling. This work paves the way for future studies on the functions of Zmiz1 and highlights the importance of combining analysis of mouse models and human data.

Published

2024

2. Development of a framework for the prediction of slope stability using machine learning paradigms

Author

Rajan, K. C., Aryal, Milan, Sharma, Keshab, Bhandary, Netra Prakash, Pokhrel, Richa, and Acharya, Indra Prasad

Published

2024

3. Endothelial cell polarity and extracellular matrix composition require functional ATP6AP2 during developmental and pathological angiogenesis

Author

Nehal R. Patel, Rajan K C, Avery Blanks, Yisu Li, Minolfa C. Prieto, and Stryder M. Meadows

Subjects

Oxygen, Mice, Proton-Translocating ATPases, Neovascularization, Pathologic, Renin, Animals, Cell Polarity, Endothelial Cells, Receptors, Cell Surface, General Medicine, Extracellular Matrix

Abstract

The (Pro)renin receptor ([P]RR), also known as ATP6AP2, is a single-transmembrane protein that is implicated in a multitude of biological processes. However, the exact role of ATP6AP2 during blood vessel development remains largely undefined. Here, we use an inducible endothelial cell-specific (EC-specific) Atp6ap2-KO mouse model to investigate the role of ATP6AP2 during both physiological and pathological angiogenesis in vivo. We observed that postnatal deletion of Atp6ap2 in ECs results in cell migration defects, loss of tip cell polarity, and subsequent impairment of retinal angiogenesis. In vitro, Atp6ap2-deficient ECs similarly displayed reduced cell migration, impaired sprouting, and defective cell polarity. Transcriptional profiling of ECs isolated from Atp6ap2 mutant mice further indicated regulatory roles in angiogenesis, cell migration, and extracellular matrix composition. Mechanistically, we provided evidence that expression of various extracellular matrix components is controlled by ATP6AP2 via the ERK pathway. Furthermore, Atp6ap2-deficient retinas exhibited reduced revascularization in an oxygen-induced retinopathy model. Collectively, our results demonstrate a critical role of ATP6AP2 as a regulator of developmental and pathological angiogenesis.

Published

2022

4. Construction and Analysis of a Colorectal Cancer Prognostic Model Based on N6-Methyladenosine-Related lncRNAs

Author

Zeng, Hanqian, primary, Xu, Yiying, additional, Xu, Shiwen, additional, Jin, Linli, additional, Shen, Yanyan, additional, Rajan, K. C., additional, Bhandari, Adheesh, additional, and Xia, Erjie, additional

Published

2021

5. Thyroid function during a prolonged stay in Antarctica

Author

Sawhney, R. C., Malhotra, A. S., Nair, C. S., Bajaj, A. C., Rajan, K. C., Pal, K., Prasad, R., and Basu, Minakshi

Published

1995

6. Human, Wildlife and Climate Change Interaction in Upper Mustang, a Himalayan Region

Author

Rajan K C

Subjects

Geography, Ecology, Wildlife, Climate change

Published

2018

7. Process development studies for the recovery of uranium and sodium sulphate from a low-grade dolostone hosted stratabound type uranium ore deposit

Author

Suri, A. K., primary, Sreenivas, T., additional, Anand Rao, K., additional, Rajan, K. C., additional, Srinivas, K., additional, Singh, A. K., additional, Shenoy, K. T., additional, Mishra, T., additional, Padmanabhan, N. P. H., additional, and Ghosh, S. K., additional

Published

2014

8. Zmiz1 is a novel regulator of lymphatic endothelial cell gene expression and function.

Author

Rajan K C, Nehal R Patel, Anoushka Shenoy, Joshua P Scallan, Mark Y Chiang, Maria J Galazo, and Stryder M Meadows

Subjects

Medicine, Science

Abstract

Zinc Finger MIZ-Type Containing 1 (Zmiz1), also known as ZIMP10 or RAI17, is a transcription cofactor and member of the Protein Inhibitor of Activated STAT (PIAS) family of proteins. Zmiz1 is critical for a variety of biological processes including vascular development. However, its role in the lymphatic vasculature is unknown. In this study, we utilized human dermal lymphatic endothelial cells (HDLECs) and an inducible, lymphatic endothelial cell (LEC)-specific Zmiz1 knockout mouse model to investigate the role of Zmiz1 in LECs. Transcriptional profiling of ZMIZ1-deficient HDLECs revealed downregulation of genes crucial for lymphatic vessel development. Additionally, our findings demonstrated that loss of Zmiz1 results in reduced expression of proliferation and migration genes in HDLECs and reduced proliferation and migration in vitro. We also presented evidence that Zmiz1 regulates Prox1 expression in vitro and in vivo by modulating chromatin accessibility at Prox1 regulatory regions. Furthermore, we observed that loss of Zmiz1 in mesenteric lymphatic vessels significantly reduced valve density. Collectively, our results highlight a novel role of Zmiz1 in LECs and as a transcriptional regulator of Prox1, shedding light on a previously unknown regulatory factor in lymphatic vascular biology.

Published

2024

9. Endothelial Zmiz1 modulates physiological and pathophysiological angiogenesis during retinal development.

Author

Patel NR, Rajan KC, Chiang MY, and Meadows SM

Abstract

Angiogenesis is a highly coordinated process involving the control of various endothelial cell behaviors. Mechanisms for transcription factor involvement in the regulation of endothelial cell dynamics and angiogenesis have become better understood, however much remains unknown, especially the role of non-DNA binding transcriptional cofactors. Here, we show that Zmiz1, a transcription cofactor, is enriched in the endothelium and critical for embryonic vascular development, postnatal retinal angiogenesis, and pathological angiogenesis in oxygen induced retinopathy (OIR). In mice, endothelial cell-specific deletion of Zmiz1 during embryogenesis led to lethality due to abnormal angiogenesis and vascular defects. Inducible endothelial cell-specific ablation of Zmiz1 postnatally resulted in impaired retinal vascular outgrowth, decreased vascular density, and increased vessel regression. In addition, angiogenic sprouting in the superficial and deep layers of the retina was markedly reduced. Correspondingly, vascular sprouting in fibrin bead assays was significantly reduced in the absence of Zmiz1, while further in vitro and in vivo evidence also suggested deficits in EC migration. In agreement with the defective sprouting angiogenesis phenotype, gene expression analysis of isolated retinal endothelial cells revealed downregulation of tip-cell enriched genes upon inactivation of Zmiz1 . Lastly, our study suggested that endothelial Zmiz1 is critical for intraretinal revascularization following hypoxia exposure in the OIR model. Taken together, these findings begin to define the previously unspecified role of endothelial Zmiz1 in physiological and pathological angiogenesis., Competing Interests: Conflict of interest: The authors have declared that no conflict of interest exists.

Published

2024

10. Zmiz1 is a novel regulator of lymphatic endothelial cell gene expression and function.

Author

Rajan KC, Patel NR, Shenoy A, Scallan JP, Chiang MY, Galazo MJ, and Meadows SM

Abstract

Zinc Finger MIZ-Type Containing 1 (Zmiz1), also known as ZIMP10 or RAI17, is a transcription cofactor and member of the Protein Inhibitor of Activated STAT (PIAS) family of proteins. Zmiz1 is critical for a variety of biological processes including vascular development. However, its role in the lymphatic vasculature is unknown. In this study, we utilized human dermal lymphatic endothelial cells (HDLECs) and an inducible, lymphatic endothelial cell (LEC)-specific Zmiz1 knockout mouse model to investigate the role of Zmiz1 in LECs. Transcriptional profiling of Zmiz1 -deficient HDLECs revealed downregulation of genes crucial for lymphatic vessel development. Additionally, our findings demonstrated that loss of Zmiz1 results in reduced expression of proliferation and migration genes in HDLECs and reduced proliferation and migration in vitro . We also presented evidence that Zmiz1 regulates Prox1 expression in vitro and in vivo by modulating chromatin accessibility at Prox1 regulatory regions. Furthermore, we observed that loss of Zmiz1 in mesenteric lymphatic vessels significantly reduced valve density. Collectively, our results highlight a novel role of Zmiz1 in LECs and as a transcriptional regulator of Prox1, shedding light on a previously unknown regulatory factor in lymphatic vascular biology., Competing Interests: Conflict of interest: The authors have declared that no conflict of interest exists. Declaration of competing interest The authors declare that they have no known competing financial interests or personal associations or relationships.

Published

2023