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A myeloid program associated with COVID-19 severity is decreased by therapeutic blockade of IL-6 signaling
- Hackney, Jason A;
- Shivram, Haridha;
- Vander Heiden, Jason;
- Overall, Chris;
- Orozco, Luz;
- Gao, Xia;
- Kim, Eugene;
- West, Nathan;
- Qamra, Aditi;
- Chang, Diana;
- Chakrabarti, Arindam;
- Choy, David F;
- Combes, Alexis J;
- Courau, Tristan;
- Fragiadakis, Gabriela K;
- Rao, Arjun Arkal;
- Ray, Arja;
- Tsui, Jessica;
- Hu, Kenneth;
- Kuhn, Nicholas F;
- Krummel, Matthew F;
- Erle, David J;
- Kangelaris, Kirsten;
- Sarma, Aartik;
- Lyon, Zoe;
- Calfee, Carolyn S;
- Woodruff, Prescott G;
- Ghale, Rajani;
- Mick, Eran;
- Byrne, Ashley;
- Zha, Beth Shoshana;
- Langelier, Charles;
- Hendrickson, Carolyn M;
- van der Wijst, Monique GP;
- Hartoularos, George C;
- Grant, Tianna;
- Bueno, Raymund;
- Lee, David S;
- Greenland, John R;
- Sun, Yang;
- Perez, Richard;
- Ogorodnikov, Anton;
- Ward, Alyssa;
- Ye, Chun Jimmie;
- Consortium, UCSF COMET;
- Abe-Jones, Yumiko;
- Adkisson, Michael;
- Ansel, K Mark;
- Asthana, Saurabh;
- Beagle, Alexander;
- Bhide, Sharvari;
- Cai, Cathy;
- Caldera, Saharai;
- Calvo, Maria;
- Carrillo, Sidney A;
- Chak, Suzanna;
- Christenson, Stephanie;
- Collins, Zachary;
- Darmanis, Spyros;
- Detweiler, Angela;
- DeVoe, Catherine;
- Eckalbar, Walter;
- Giberson, Jeremy;
- Gonzalez, Ana;
- Gordon, Gracie;
- Serpa, Paula Hayakawa;
- Jauregui, Alejandra;
- Jones, Chayse;
- Ke, Serena;
- Kushnoor, Divya;
- Lea, Tasha;
- Lee, Deanna;
- Leligdowicz, Aleksandra;
- Liu, Yale;
- Mahboob, Salman;
- Maliskova, Lenka;
- Matthay, Michael;
- McCarthy, Elizabeth;
- Muñoz-Sandoval, Priscila;
- Neff, Norma;
- Nguyen, Viet;
- Nigam, Nishita;
- Parada, Randy;
- Phelps, Maira;
- Pierce, Logan;
- Prasad, Priya;
- Rashid, Sadeed;
- Reeder, Gabriella;
- Rodriguez, Nicklaus;
- Samad, Bushra;
- Schroeder, Andrew;
- Shaw, Cole;
- Shen, Alan;
- Sigman, Austin;
- Sinha, Pratik;
- Spitzer, Matthew;
- Sunshine, Sara;
- Tang, Kevin;
- Altamirano, Luz Torres;
- Tsitsiklis, Alexandra;
- Tumurbaatar, Erden;
- Upadhyay, Vaibhav;
- Whatley, Alexander;
- Willmore, Andrew;
- Wilson, Michael;
- Winkler, Juliane;
- Wong, Kristine;
- Yee, Kimberly;
- Yu, Michelle;
- Zhou, Mingyue;
- Zhu, Wandi S;
- Ramalingam, Thiru;
- McBride, Jacqueline M;
- Cai, Fang;
- Teterina, Anastasia;
- Bao, Min;
- Tsai, Larry;
- Rosas, Ivan O;
- Regev, Aviv;
- Kapadia, Sharookh B;
- Bauer, Rebecca N;
- Rosenberger, Carrie M
- et al.
Published Web Location
https://doi.org/10.1016/j.isci.2023.107813Abstract
Altered myeloid inflammation and lymphopenia are hallmarks of severe infections. We identified the upregulated EN-RAGE gene program in airway and blood myeloid cells from patients with acute lung injury from SARS-CoV-2 or other causes across 7 cohorts. This program was associated with greater clinical severity and predicted future mechanical ventilation and death. EN-RAGEhi myeloid cells express features consistent with suppressor cell functionality, including low HLA-DR and high PD-L1. Sustained EN-RAGE program expression in airway and blood myeloid cells correlated with clinical severity and increasing expression of T cell dysfunction markers. IL-6 upregulated many EN-RAGE program genes in monocytes in vitro. IL-6 signaling blockade by tocilizumab in a placebo-controlled clinical trial led to rapid normalization of EN-RAGE and T cell gene expression. This identifies IL-6 as a key driver of myeloid dysregulation associated with worse clinical outcomes in COVID-19 patients and provides insights into shared pathophysiological mechanisms in non-COVID-19 ARDS.
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