Literature DB >> 30232287

Haptoglobin improves shock, lung injury, and survival in canine pneumonia.

Kenneth E Remy1,2, Irene Cortés-Puch1, Steven B Solomon1, Junfeng Sun1, Benjamin M Pockros1, Jing Feng1, Juan J Lertora3, Roy R Hantgan4, Xiaohua Liu5, Andreas Perlegas5, H Shaw Warren6, Mark T Gladwin7, Daniel B Kim-Shapiro5, Harvey G Klein8, Charles Natanson1.   

Abstract

During the last half-century, numerous antiinflammatory agents were tested in dozens of clinical trials and have proven ineffective for treating septic shock. The observation in multiple studies that cell-free hemoglobin (CFH) levels are elevated during clinical sepsis and that the degree of increase correlates with higher mortality suggests an alternative approach. Human haptoglobin binds CFH with high affinity and, therefore, can potentially reduce iron availability and oxidative activity. CFH levels are elevated over approximately 24-48 hours in our antibiotic-treated canine model of S. aureus pneumonia that simulates the cardiovascular abnormalities of human septic shock. In this 96-hour model, resuscitative treatments, mechanical ventilation, sedation, and continuous care are translatable to management in human intensive care units. We found, in this S. aureus pneumonia model inducing septic shock, that commercial human haptoglobin concentrate infusions over 48-hours bind canine CFH, increase CFH clearance, and lower circulating iron. Over the 96-hour study, this treatment was associated with an improved metabolic profile (pH, lactate), less lung injury, reversal of shock, and increased survival. Haptoglobin binding compartmentalized CFH to the intravascular space. This observation, in combination with increasing CFHs clearance, reduced available iron as a potential source of bacterial nutrition while decreasing the ability for CFH and iron to cause extravascular oxidative tissue injury. In contrast, haptoglobin therapy had no measurable antiinflammatory effect on elevations in proinflammatory C-reactive protein and cytokine levels. Haptoglobin therapy enhances normal host defense mechanisms in contrast to previously studied antiinflammatory sepsis therapies, making it a biologically plausible novel approach to treat septic shock.

Entities:  

Keywords:  Bacterial infections; Clinical Trials; Drug therapy; Infectious disease; Innate immunity

Mesh:

Substances:

Year:  2018        PMID: 30232287      PMCID: PMC6237235          DOI: 10.1172/jci.insight.123013

Source DB:  PubMed          Journal:  JCI Insight        ISSN: 2379-3708


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2.  Haptoglobin-2 variant increases susceptibility to acute respiratory distress syndrome during sepsis.

Authors:  V Eric Kerchberger; Julie A Bastarache; Ciara M Shaver; Hiromasa Nagata; J Brennan McNeil; Stuart R Landstreet; Nathan D Putz; Wen-Kuang Yu; Jordan Jesse; Nancy E Wickersham; Tatiana N Sidorova; David R Janz; Chirag R Parikh; Edward D Siew; Lorraine B Ware
Journal:  JCI Insight       Date:  2019-11-01

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4.  Toxic effects of cell-free hemoglobin on the microvascular endothelium: implications for pulmonary and nonpulmonary organ dysfunction.

Authors:  Jamie E Meegan; Julie A Bastarache; Lorraine B Ware
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Review 5.  Extracellular HMGB1: a therapeutic target in severe pulmonary inflammation including COVID-19?

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Journal:  Mol Med       Date:  2020-05-07       Impact factor: 6.354

6.  Iron overload causes a mild and transient increase in acute lung injury.

Authors:  Vida Zhang; Tomas Ganz; Elizabeta Nemeth; Airie Kim
Journal:  Physiol Rep       Date:  2020-06

7.  Ferritin Light Chain Confers Protection Against Sepsis-Induced Inflammation and Organ Injury.

Authors:  Abolfazl Zarjou; Laurence M Black; Kayla R McCullough; Travis D Hull; Stephanie K Esman; Ravindra Boddu; Sooryanarayana Varambally; Darshan S Chandrashekar; Wenguang Feng; Paolo Arosio; Maura Poli; Jozsef Balla; Subhashini Bolisetty
Journal:  Front Immunol       Date:  2019-02-04       Impact factor: 7.561

8.  Haptoglobin therapy has differential effects depending on severity of canine septic shock and cell-free hemoglobin level.

Authors:  Kenneth E Remy; Irene Cortés-Puch; Junfeng Sun; Jing Feng; Juan J Lertora; Thomas Risoleo; Julia Katz; Swati Basu; Xiaohua Liu; Andreas Perlegas; Daniel B Kim-Shapiro; Harvey G Klein; Charles Natanson; Steven B Solomon
Journal:  Transfusion       Date:  2019-10-22       Impact factor: 3.337

Review 9.  Targeting Inflammation Driven by HMGB1.

Authors:  Huan Yang; Haichao Wang; Ulf Andersson
Journal:  Front Immunol       Date:  2020-03-20       Impact factor: 7.561

10.  Emerging pharmacological therapies for ARDS: COVID-19 and beyond.

Authors:  Shahd Horie; Bairbre McNicholas; Emanuele Rezoagli; Tài Pham; Ger Curley; Danny McAuley; Cecilia O'Kane; Alistair Nichol; Claudia Dos Santos; Patricia R M Rocco; Giacomo Bellani; John G Laffey
Journal:  Intensive Care Med       Date:  2020-07-11       Impact factor: 41.787

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