4.5 Article

Salvage of focal cerebral ischemic damage by transfusion of high O2-affinity recombinant hemoglobin polymers in mouse

Journal

JOURNAL OF APPLIED PHYSIOLOGY
Volume 100, Issue 5, Pages 1688-1691

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/japplphysiol.01374.2005

Keywords

blood substitute; cerebral ischemia; middle cerebral artery; oxygen carrier

Funding

  1. NINDS NIH HHS [NS-38684, R01 NS038684] Funding Source: Medline

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Cellfree hemoglobin solutions with high oxygen affinity might be beneficial for selectively delivering oxygen to ischemic tissue. A recombinant hybrid hemoglobin molecule was designed using the human alpha-subunit and the bovine beta-subunit, with placement of surface cysteines to permit disulfide bond polymerization of the tetramers. The resulting protein generated from an Escherichia coli expression system had a molecular mass > 1 MDa, a P-50 of similar to 3 Torr, and a cooperativity of n = 1.0. Anesthetized mice were transfused during 2-h occlusion of the middle cerebral artery. Compared with transfusion with 5% albumin, cerebral infarct volume was reduced by 41% with transfusion of a 3% solution of the high oxygen-affinity hemoglobin polymer and by 50% with transfusion of a 6% solution of the polymer. Transfusion of a 6% solution of a 500-kDa polymer possessing a P50 of 17 Torr and a cooperativity of n = 2.0 resulted in a 66% reduction of infarct volume. These results indicate that cell-free Hb polymers with P-50 values much lower than that of red blood cell hemoglobin are highly capable of salvaging ischemic brain. The assumption that the P-50 of blood substitutes should be similar to that of blood might not be warranted when used during ischemic conditions.

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