Your search keyword '"Harms, Paul W."' showing total 5 results

1. Single-cell sequencing reveals Hippo signaling as a driver of fibrosis in hidradenitis suppurativa

Author

van Straalen, Kelsey R., Ma, Feiyang, Tsou, Pei-Suen, Plazyo, Olesya, Gharaee-Kermani, Mehrnaz, Calbet, Marta, Xing, Xianying, Sarkar, Mrinal K., Uppala, Ranjitha, Harms, Paul W., Wasikowski, Rachael, Nahlawi, Lina, Nakamura, Mio, Eshaq, Milad, Wang, Cong, Dobry, Craig, Kozlow, Jeffrey H., Cherry-Bukowiec, Jill, Brodie, William D., Wolk, Kerstin, Uluckan, Ozge, Mattichak, Megan N., Pellegrini, Matteo, Modlin, Robert L., Maverakis, Emanual, Sabat, Robert, Kahlenberg, J. Michelle, Billi, Allison C., Tsoi, Lam C., and Gudjonsson, Johann E.

Subjects

Verteporfin, Fibrosis, RNA sequencing, Immune response, B cells, Adalimumab, Health care industry, University of Michigan. Medical School

Abstract

Hidradenitis suppurativa (HS) is a chronic inflammatory disease characterized by abscesses, nodules, dissecting/ draining tunnels, and extensive fibrosis. Here, we integrate single-cell RNA sequencing, spatial transcriptomics, and immunostaining to provide an unprecedented view of the pathogenesis of chronic HS, characterizing the main cellular players and defining their interactions. We found a striking layering of the chronic HS infiltrate and identified the contribution of 2 fibroblast subtypes ([SFRP4.sup.+] and [CXCL13.sup.+]) in orchestrating this compartmentalized immune response. We further demonstrated the central role of the Hippo pathway in promoting extensive fibrosis in HS and provided preclinical evidence that the profibrotic fibroblast response in HS can be modulated through inhibition of this pathway. These data provide insights into key aspects of HS pathogenesis with broad therapeutic implications., Introduction Hidradenitis suppurativa (HS) is a chronic inflammatory disease of the skin that affects 1% of the general population (1). The disease is characterized by acute, recurrent inflammatory nodules and [...]

Published

2024

2. Single cell sequencing reveals Hippo signaling as a driver of fibrosis in hidradenitis suppurativa

Author

van Straalen, Kelsey R., primary, Ma, Feiyang, additional, Tsou, Pei-Suen, additional, Plazyo, Olesya, additional, Gharaee-Kermani, Mehrnaz, additional, Calbet, Marta, additional, Xing, Xianying, additional, Sarkar, Mrinal K., additional, Uppala, Ranjitha, additional, Harms, Paul W., additional, Wasikowski, Rachael, additional, Nahlawi, Lina, additional, Nakamura, Mio, additional, Eshaq, Milad, additional, Wang, Cong, additional, Dobry, Craig J., additional, Kozlow, Jeffrey H., additional, Cherry-Bukowiec, Jill R., additional, Brodie, William D., additional, Wolk, Kerstin, additional, Uluckan, Özge, additional, Mattichak, Megan N., additional, Pellegrini, Matteo, additional, Modlin, Robert L., additional, Maverakis, Emanual, additional, Sabat, Robert, additional, Kahlenberg, J. Michelle, additional, Billi, Allison C., additional, Tsoi, Lam C., additional, and Gudjonsson, Johann E., additional

Published

2023

3. Direct cellular reprogramming enables development of viral T antigen-driven Merkel cell carcinoma in mice

Author

Verhaegen, Monique E., Harms, Paul W., Van Goor, Julia J., Arche, Jacob, Patrick, Matthew T., Wilbert, Dawn, Zabawa, Haley, Grachtchouk, Marina, Liu, Chia-Jen, Hu, Kevin, Kelly, Michael C., Chen, Ping, Saunders, Thomas L., Weidinger, Stephan, Syu, Li-Jyun, Runge, John S., Gudjonsson, Johann E., Wong, Sunny Y., Brownell, Isaac, Cieslik, Marcin, Udager, Aaron M., Chinnaiyan, Arul M., Tsoi, Lam C., and Dlugosz, Andrzej A.

Subjects

Oncology, Experimental, Merkel cell carcinoma -- Genetic aspects -- Development and progression, Viral antigens -- Genetic aspects, Gene expression -- Research, Cell differentiation -- Research, Tumor antigens -- Genetic aspects, Cancer -- Research, Health care industry

Abstract

Merkel cell carcinoma (MCC) is an aggressive neuroendocrine skin cancer that frequently carries an integrated Merkel cell polyomavirus (MCPyV) genome and expresses viral transforming antigens (TAgs). MCC tumor cells also express signature genes detected in skin-resident, postmitotic Merkel cells, including atonal bHLH transcription factor 1 (ATOH1), which is required for Merkel cell development from epidermal progenitors. We now report the use of in vivo cellular reprogramming, using ATOH1, to drive MCC development from murine epidermis. We generated mice that conditionally expressed MCPyV TAgs and ATOH1 in epidermal cells, yielding microscopic collections of proliferating MCC-like cells arising from hair follicles. Immunostaining of these nascent tumors revealed p53 accumulation and apoptosis, and targeted deletion of transformation related protein 53 (Trp53) led to development of gross skin tumors with classic MCC histology and marker expression. Global transcriptome analysis confirmed the close similarity of mouse and human MCCs, and hierarchical clustering showed conserved upregulation of signature genes. Our data establish that expression of MCPyV TAgs in ATOH1-reprogrammed epidermal cells and their neuroendocrine progeny initiates hair follicle-derived MCC tumorigenesis in adult mice. Moreover, progression to full-blown MCC in this model requires loss of p53, mimicking the functional inhibition of p53 reported in human MCPyV-positive MCCs., Introduction Merkel cell carcinoma (MCC) is an aggressive neuroendocrine skin tumor with a poor prognosis (1), although up to 50% of patients with advanced disease respond to immunotherapy (2). In [...]

Published

2022

4. Translational implications of Th17-skewed inflammation due to genetic deficiency of a cadherin stress sensor

Author

Godsel, Lisa M., Roth-Carter, Quinn R., Koetsier, Jennifer L., Tsoi, Lam C., Huffine, Amber L., Broussard, Joshua A., Fitz, Gillian N., Lloyd, Sarah M., Kweon, Junghun, Burks, Hope E., Hegazy, Marihan, Amagai, Saki, Harms, Paul W., Xing, Xianying, Kirma, Joseph, Johnson, Jodi L., Urciuoli, Gloria, Doglio, Lynn T., Swindell, William R., Awatramani, Rajeshwar, Sprecher, Eli, Bao, Xiaomin, Cohen-Barak, Eran, Missero, Caterina, Gudjonsson, Johann E., and Green, Kathleen J.

Subjects

Genetic translation -- Health aspects, Cadherins -- Physiological aspects -- Health aspects, CD4 lymphocytes -- Genetic aspects -- Health aspects, Skin lesions -- Models -- Genetic aspects -- Physiological aspects, Health care industry

Abstract

Desmoglein 1 (Dsg1) is a cadherin restricted to stratified tissues of terrestrial vertebrates, which serve as essential physical and immune barriers. Dsg1 loss-of-function mutations in humans result in skin lesions and multiple allergies, and isolated patient keratinocytes exhibit increased proallergic cytokine expression. However, the mechanism by which genetic deficiency of Dsg1 causes chronic inflammation is unknown. To determine the systemic response to Dsg1 loss, we deleted the 3 tandem Dsg1 genes in mice. Whole transcriptome analysis of embryonic [Dsg1.sup.-/-] skin showed a delay in expression of adhesion/differentiation/ keratinization genes at E17.5, a subset of which recovered or increased by E18.5. Comparing epidermal transcriptomes from Dsg1-deficient mice and humans revealed a shared IL-17-skewed inflammatory signature. Although the impaired intercellular adhesion observed in [Dsg1.sup.-/-] mice resembles that resulting from anti-Dsg1 pemphigus foliaceus antibodies, pemphigus skin lesions exhibit a weaker IL-17 signature. Consistent with the clinical importance of these findings, treatment of 2 Dsg1-deficient patients with an IL-12/IL-23 antagonist originally developed for psoriasis resulted in improvement of skin lesions. Thus, beyond impairing the physical barrier, loss of Dsg1 function through gene mutation results in a psoriatic-like inflammatory signature before birth, and treatment with a targeted therapy significantly improved skin lesions in patients., Introduction The multilayered epidermal barrier is made up of interdependent microbiome, chemical, physical, and immune components. These components work together to protect against water loss, physical insults, and infection (1, [...]

Published

2022

5. Host expression of PD-L1 determines efficacy of PD-L1 pathway blockade-mediated tumor regression

Author

Lin, Heng, Wei, Shuang, Hurt, Elaine M., Green, Michael D., Zhao, Lili, Vatan, Linda, Szeliga, Wojciech, Herbst, Ronald, Harms, Paul W., Fecher, Leslie A., Vats, Pankaj, Chinnaiyan, Arul M., Lao, Christopher D., Lawrence, Theodore S., Wicha, Max, Hamanishi, Junzo, Mandai, Masaki, Kryczek, Ilona, and Zou, Weiping

Subjects

Apoptosis -- Health aspects, Cancer regression -- Genetic aspects, Ligands (Biochemistry) -- Health aspects, Health care industry

Abstract

Programmed death-1 receptor (PD-L1, B7-H1) and programmed cell death protein 1 (PD-1) pathway blockade is a promising therapy for treating cancer. However, the mechanistic contribution of host and tumor PD-L1 and PD-1 signaling to the therapeutic efficacy of PD-L1 and PD-1 blockade remains elusive. Here, we evaluated 3 tumor-bearing mouse models that differ in their sensitivity to PD-L1 blockade and demonstrated a loss of therapeutic efficacy of PD-L1 blockade in immunodeficient mice and in PD-L1- and PD-1-deficient mice. In contrast, neither knockout nor overexpression of PD-L1 in tumor cells had an effect on PD-L1 blockade efficacy. Human and murine studies showed high levels of functional PD-L1 expression in dendritic cells and macrophages in the tumor microenvironments and draining lymph nodes. Additionally, expression of PD-L1 on dendritic cells and macrophages in ovarian cancer and melanoma patients correlated with the efficacy of treatment with either anti-PD-1 alone or in combination with anti-CTLA-4. Thus, PD-L1-expressing dendritic cells and macrophages may mechanistically shape and therapeutically predict clinical efficacy of PD-L1/PD-1 blockade., Introduction Therapeutic blockade of programmed death-ligand 1 (PD-L1, B7-H1) or programmed death-1 receptor (PD-1) with mAbs leads to durable tumor control in a minority of patients across many cancer histologies [...]

Published

2018