Your search keyword '"Uppala, Ranjitha"' showing total 5 results

1. Atopic Dermatitis Is an IL-13–Dominant Disease with Greater Molecular Heterogeneity Compared to Psoriasis

Author

Tsoi, Lam C., Rodriguez, Elke, Degenhardt, Frauke, Baurecht, Hansjörg, Wehkamp, Ulrike, Volks, Natalie, Szymczak, Silke, Swindell, William R., Sarkar, Mrinal K., Raja, Kalpana, Shao, Shuai, Patrick, Matthew, Gao, Yilin, Uppala, Ranjitha, Perez White, Bethany E, Getsios, Spiro, Harms, Paul W., Maverakis, Emanual, Elder, James T., Franke, Andre, Gudjonsson, Johann E., and Weidinger, Stephan

Abstract

Atopic dermatitis (AD) affects up to 20% of children and adults worldwide. To gain a deeper understanding of the pathophysiology of AD, we conducted a large-scale transcriptomic study of AD with deeply sequenced RNA-sequencing samples using long (126-bp) paired-end reads. In addition to the comparisons against previous transcriptomic studies, we conducted in-depth analysis to obtain a high-resolution view of the global architecture of the AD transcriptome and contrasted it with that of psoriasis from the same cohort. By using 147 RNA samples in total, we found striking correlation between dysregulated genes in lesional psoriasis and lesional AD skin with 81% of AD dysregulated genes being shared with psoriasis. However, we described disease-specific molecular and cellular features, with AD skin showing dominance of IL-13 pathways, but with near undetectable IL-4 expression. We also demonstrated greater disease heterogeneity and larger proportion of dysregulated long noncoding RNAs in AD, and illustrated the translational impact, including skin-type classification and drug-target prediction. This study is by far the largest study comparing the AD and psoriasis transcriptomes using RNA sequencing and demonstrating the shared inflammatory components, as well as specific discordant cytokine signatures of these two skin diseases.

Published

2019

2. Noninvasive Tape-Stripping with High-Resolution RNA Profiling Effectively Captures a Preinflammatory State in Nonlesional Psoriatic Skin

Author

Tsoi, Lam C., Xing, Xianying, Xing, Enze, Wasikowski, Rachael, Shao, Shuai, Zeng, Chang, Plazyo, Olesya, Kirma, Joseph, Jiang, Yanyung, Billi, Allison C., Sarkar, Mrinal K., Turnier, Jessica L., Uppala, Ranjitha, Smith, Kathleen M., Helfrich, Yolanda, Voorhees, John J., Maverakis, Emanual, Modlin, Robert L., Kahlenberg, J. Michelle, Scott, Victoria E., and Gudjonsson, Johann E.

Abstract

Tape stripping is a minimally invasive, nonscarring method that can be utilized to assess gene expression in the skin but is infrequently used given technical constraints. By comparing different tape stripping technologies and full-thickness skin biopsy results of lesional and nonlesional psoriatic skin from the same patients, we demonstrate that tape stripping with optimized high-resolution transcriptomic profiling can be used to effectively assess and characterize inflammatory responses in the skin. Upon comparison with single-cell RNA-sequencing data from psoriatic full-thickness skin biopsies, we illustrate that tape-stripping efficiently captures the transcriptome of the upper layers of the epidermis with sufficient resolution to assess the molecular components of the feed-forward immune amplification pathway in psoriasis. Notably, nonlesional psoriatic skin sampled by tape stripping demonstrates activated, proinflammatory changes when compared to healthy control skin, suggesting a prepsoriatic state, which is not captured on full-thickness skin biopsy transcriptome profiling. This work illustrates an approach to assess inflammatory response in the epidermis by combining noninvasive sampling with high throughput RNA-sequencing, providing a foundation for biomarker discoveries and mechanism of action studies for inflammatory skin conditions.

Published

2022

3. NIX initiates mitochondrial fragmentation via DRP1 to drive epidermal differentiation

Author

Simpson, Cory L., Tokito, Mariko K., Uppala, Ranjitha, Sarkar, Mrinal K., Gudjonsson, Johann E., and Holzbaur, Erika L.F.

Abstract

The epidermis regenerates continually to maintain a protective barrier at the body’s surface composed of differentiating keratinocytes. Maturation of this stratified tissue requires that keratinocytes undergo wholesale organelle degradation upon reaching the outermost tissue layers to form compacted, anucleate cells. Through live imaging of organotypic cultures of human epidermis, we find that regulated breakdown of mitochondria is critical for epidermal development. Keratinocytes in the upper layers initiate mitochondrial fragmentation, depolarization, and acidification upon upregulating the mitochondrion-tethered autophagy receptor NIX. Depleting NIX compromises epidermal maturation and impairs mitochondrial elimination, whereas ectopic NIX expression accelerates keratinocyte differentiation and induces premature mitochondrial fragmentation via the guanosine triphosphatase (GTPase) DRP1. We further demonstrate that inhibiting DRP1 blocks NIX-mediated mitochondrial breakdown and disrupts epidermal development. Our findings establish mitochondrial degradation as a key step in terminal keratinocyte differentiation and define a pathway operating via the mitophagy receptor NIX in concert with DRP1 to drive epidermal morphogenesis.

Published

2021

4. IRAK2 Has a Critical Role in Promoting Feed-Forward Amplification of Epidermal Inflammatory Responses

Author

Shao, Shuai, Tsoi, Lam C., Swindell, William R., Chen, Jiaoling, Uppala, Ranjitha, Billi, Allison C., Xing, Xianying, Zeng, Chang, Sarkar, Mrinal K., Wasikowski, Rachael, Jiang, Yanyun, Kirma, Joseph, Sun, Jingru, Plazyo, Olesya, Wang, Gang, Harms, Paul W., Voorhees, John J., Ward, Nicole L., Ma, Feiyang, Pellegrini, Matteo, Merleev, Alexander, Perez White, Bethany E., Modlin, Robert L., Andersen, Bogi, Maverakis, Emanual, Weidinger, Stephan, Kahlenberg, J. Michelle, and Gudjonsson, Johann E.

Abstract

Many inflammatory skin diseases are characterized by altered epidermal differentiation. Whether this altered differentiation promotes inflammatory responses has been unknown. Here, we show that IRAK2, a member of the signaling complex downstream of IL-1 and IL-36, correlates positively with disease severity in both atopic dermatitis and psoriasis. Inhibition of epidermal IRAK2 normalizes differentiation and inflammation in two mouse models of psoriasis- and atopic dermatitis–like inflammation. Specifically, we demonstrate that IRAK2 ties together proinflammatory and differentiation-dependent responses and show that this function of IRAK2 is specific to keratinocytes and acts through the differentiation-associated transcription factor ZNF750. Taken together, our findings suggest that IRAK2 has a critical role in promoting feed-forward amplification of inflammatory responses in skin through modulation of differentiation pathways and inflammatory responses.

Published

2021

5. IFN-γ enhances cell-mediated cytotoxicity against keratinocytes via JAK2/STAT1 in lichen planus

Author

Shao, Shuai, Tsoi, Lam C., Sarkar, Mrinal K., Xing, Xianying, Xue, Ke, Uppala, Ranjitha, Berthier, Celine C., Zeng, Chang, Patrick, Matthew, Billi, Allison C., Fullmer, Joseph, Beamer, Maria A., Perez-White, Bethany, Getsios, Spiro, Schuler, Andrew, Voorhees, John J., Choi, Sung, Harms, Paul, Kahlenberg, J. Michelle, and Gudjonsson, Johann E.

Abstract

IFN-γ enhances keratinocyte death in lichen planus.

Published

2019