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Citations to this article

Activation of MDL-1 (CLEC5A) on immature myeloid cells triggers lethal shock in mice
Ricky Cheung, … , Paul G. Heyworth, Robert H. Pierce
Ricky Cheung, … , Paul G. Heyworth, Robert H. Pierce
Published October 17, 2011
Citation Information: J Clin Invest. 2011;121(11):4446-4461. https://doi.org/10.1172/JCI57682.
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Research Article Article has an altmetric score of 7

Activation of MDL-1 (CLEC5A) on immature myeloid cells triggers lethal shock in mice

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Abstract

Systemic inflammatory response syndrome (SIRS) is a potentially lethal condition, as it can progress to shock, multi-organ failure, and death. It can be triggered by infection, tissue damage, or hemorrhage. The role of tissue injury in the progression from SIRS to shock is incompletely understood. Here, we show that treatment of mice with concanavalin A (ConA) to induce liver injury triggered a G-CSF–dependent hepatic infiltration of CD11b+Gr-1+Ly6G+Ly6C+ immature myeloid cells that expressed the orphan receptor myeloid DAP12–associated lectin–1 (MDL-1; also known as CLEC5A). Activation of MDL-1 using dengue virus or an agonist MDL-1–specific antibody in the ConA-treated mice resulted in shock. The MDL-1+ cells were pathogenic, and in vivo depletion of MDL-1+ cells provided protection. Triggering MDL-1 on these cells induced production of NO and TNF-α, which were found to be elevated in the serum of treated mice and required for MDL-1–induced shock. Surprisingly, MDL-1–induced NO and TNF-α production required eNOS but not iNOS. Activation of DAP12, DAP10, Syk, PI3K, and Akt was critical for MDL-1–induced shock. In addition, Akt physically interacted with and activated eNOS. Therefore, triggering of MDL-1 on immature myeloid cells and production of NO and TNF-α may play a critical role in the pathogenesis of shock. Targeting the MDL-1/Syk/PI3K/Akt/eNOS pathway represents a potential new therapeutic strategy to prevent the progression of SIRS to shock.

Authors

Ricky Cheung, Fran Shen, Joseph H. Phillips, Mandy J. McGeachy, Daniel J. Cua, Paul G. Heyworth, Robert H. Pierce

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 2019 2018 2017 2016 2015 2014 2013 2012 2011 Total
Citations: 1 2 2 4 2 3 2 3 3 6 2 1 1 2 1 35
Citation information
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Citations to this article (35)

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Exploring Differentially Methylated Genes among Preterm Birth and Full-Term Birth.
Razzaq A, ElKahlout R, Nasrallah GK, Ibrahim FE, Samara M, Zayed H, Abdulrouf PV, Al-Jurf R, Najjar A, Farrell T, Qoronfleh MW, Rifai HA, Al-Dewik N
Lifestyle genomics 2025
IL-23 induces CLEC5A(+) IL-17A(+) neutrophils and elicit skin inflammation associated with psoriatic arthritis.
Furuya H, Nguyen CT, Chan T, Marusina AI, Merleev AA, Garcia-Hernandez ML, Hsieh SL, Tsokos GC, Ritchlin CT, Tagkopoulos I, Maverakis E, Adamopoulos IE
Journal of Autoimmunity 2024
The deficient CLEC5A ameliorates the behavioral and pathological deficits via the microglial Aβ clearance in Alzheimer's disease mouse model.
Lin YY, Chang WH, Hsieh SL, Cheng IH
Journal of neuroinflammation 2024
In-Silico CLEC5A mRNA expression analysis to predict Dengue susceptibility in cancer patients
Suchanti S, Stephen BJ, Chaurasia TP, Raghuwanshi AP, Singh G, Singh A, Mishra R
Biochemistry and Biophysics Reports 2023
Identification of immune-related genes in diagnosing retinopathy of prematurity with sepsis through bioinformatics analysis and machine learning
Chen H, Chen E, Lu Y, Xu Y
Frontiers in Genetics 2023
Intestinal inflammation drives MDL-1+ osteoclast precursor expansion and enhanced osteoclastogenesis to promote colitis-associated bone loss
Christopher Peek, Caleb A Ford, Kara R Eichelberger, Justin Jacobse, Teresa P Torres, Damian Maseda, Yvonne L. Latour, M. Blanca Piazuelo, joshua johnson, Mariana X Byndloss, Keith T. Wilson, Jeffrey C. Rathmell, Jeremy A. Goettel, James E Cassat
CMGH Cellular and Molecular Gastroenterology and Hepatology 2022
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Tosiek MJ, Groesser K, Pekcec A, Zwirek M, Murugesan G, Borges E
Journal of Immunology Research 2022
A Pan-Cancer Analysis Reveals CLEC5A as a Biomarker for Cancer Immunity and Prognosis
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Viruses 2022
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Menegatti S, Guillemot V, Latis E, Yahia-Cherbal H, Mittermüller D, Rouilly V, Mascia E, Rosine N, Koturan S, Millot GA, Leloup C, Duffy D, Gleizes A, Hacein-Bey-Abina S, Sellam J, Berenbaum F, Miceli-Richard C, Dougados M, Bianchi E, Rogge L
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Frontiers in immunology 2019
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Frontiers in immunology 2019
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J Sprokholt, LC Helgers, TB Geijtenbeek
Future Virology 2018
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C Schiffman, CM McHale, AE Hubbard, L Zhang, R Thomas, R Vermeulen, G Li, M Shen, SM Rappaport, S Yin, Q Lan, MT Smith, N Rothman, SD Peddada
PloS one 2018
Molecular imaging assessment of periodontitis lesions in an experimental mouse model.
Ideguchi H, Yamashiro K, Yamamoto T, Shimoe M, Hongo S, Kochi S, Yoshihara-Hirata C, Aoyagi H, Kawamura M, Takashiba S
Clinical Oral Investigations 2018
FTY720 Attenuates Angiotensin II-Induced Podocyte Damage via Inhibiting Inflammatory Cytokines
K Su, P Zeng, W Liang, Z Luo, Y Wang, X Lv, Q Han, M Yan, C Chen
Mediators of Inflammation 2017
The macrophage C-type lectin receptor CLEC5A (MDL-1) expression is associated with early plaque progression and promotes macrophage survival
W Xiong, H Wang, L Lu, R Xi, F Wang, G Gu, R Tao
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Role of TREM1-DAP12 in Renal Inflammation during Obstructive Nephropathy
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