Thrombomodulin protects against acute vascular and multiorgan injury in sickle cell disease
Guohui Ren, Dustin R. Fraidenburg, Suman Setty, Jiwang Chen, Janae Gonzales, Maria Armila Ruiz, Zalaya Ivy, Najmeh Eskandari, Richard D. Minshall, James P. Lash, Victor R. Gordeuk, Santosh L. Saraf
Guohui Ren, Dustin R. Fraidenburg, Suman Setty, Jiwang Chen, Janae Gonzales, Maria Armila Ruiz, Zalaya Ivy, Najmeh Eskandari, Richard D. Minshall, James P. Lash, Victor R. Gordeuk, Santosh L. Saraf
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Research Article Hematology Nephrology

Thrombomodulin protects against acute vascular and multiorgan injury in sickle cell disease

Abstract

Vaso-occlusive episodes (VOEs) in the setting of hyperhemolysis can rapidly evolve into multiorgan failure in sickle cell disease (SCD). Although the mechanisms for rapid progression to multiorgan failure are unclear, a systemic vasculopathy with thrombotic microangiopathy–type features has been described. Reduced thrombomodulin (TM) function is implicated in some thrombotic microangiopathy syndromes. We observed a greater decline in platelet count and hemoglobin concentration and an increase in vascular injury biomarkers within 24 hours of admission for a VOE in 12 patients with SCD with multiorgan failure versus 12 patients without multiorgan failure. We observed decreased TM expression on the lung and kidney vasculature of 3 additional patients with SCD with multiorgan failure compared with a control patient without SCD. Transgenic SCD mice challenged with cell-free hemoglobin had reduced TM function, increased vascular injury biomarkers, and reduced renal cortical blood flow. Infusion of recombinant TM 2 or 24 hours after the challenge restored cortical blood flow and mitigated increases in vascular injury, complement activation, and tubular injury biomarkers, and protected against acute kidney and lung injury. We demonstrated that impaired TM function may be involved in the systemic vasculopathy of SCD-related multiorgan failure, and infusion of recombinant TM may restore vascular function and protect against acute organ damage.

Authors

Guohui Ren, Dustin R. Fraidenburg, Suman Setty, Jiwang Chen, Janae Gonzales, Maria Armila Ruiz, Zalaya Ivy, Najmeh Eskandari, Richard D. Minshall, James P. Lash, Victor R. Gordeuk, Santosh L. Saraf

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Figure 1

Thrombotic microangiopathy–type features in patients with SCD.

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Thrombotic microangiopathy–type features in patients with SCD. Patients ...
Patients with SCD who develop multiorgan failure had a larger (A) red blood cell hemoglobin and (B) platelet count decline relative to the most recent preceding outpatient laboratory values and higher (C) VCAM-1, (D) vWF, and (E) VEGF compared with those hospitalized for a VOE without multiorgan failure by 1-way ANOVA. (F) Kidney section from a resection control (A1) and autopsy specimens of patients with SCD (A2–A4) (original magnification, ×200); stained with TM. The kidneys of patients with SCD show decreased expression (weak to moderate patchy positivity) in the endothelial cells of the glomeruli (black *), arterioles (green *), and peritubular capillaries (red *) compared with the control (A1). Lung section from a resection control (B1) and autopsy specimens of patients with SCD (B2–B4) (original magnification, 200×); stained with TM. The lungs of patients with SCD show decreased expression (weak to moderate patchy positivity) in the endothelial cells in the alveolar spaces (green asterisk) compared with the control (black asterisk) (B1).