Figure 6
Figure 6. Sickle chimeras with 10% of normal FII levels have diminished pulmonary pathology. (A-C) Representative lung sections of HbS/FIIWT mice (left panels) compared with that of HbS/FIIlox/− mice (right panels) showing: (A) increased inflammatory infiltrate in HbS/FIIWT lungs compared with HbS/FIIlox/− lungs. Objective, ×10. (B) Increased alveolar macrophages in HbS/FIIWT lungs compared with HbS/FIIlox/− lungs. Objective, ×40. (C) Increased edema around blood vessels in HbS/FIIWT lungs vs its lack in HbS/FIIlox/− lungs. Objective, ×40. Black arrows indicate the pathology described in each panel. Images are representative of 6 to 9 mice per experimental group. Mice used as transplant recipients were of similar ages (8-10 weeks) with equal numbers of males and females distributed among the experimental groups. Fully chimeric sickle or normal mice were followed for a year posttransplantation.

Sickle chimeras with 10% of normal FII levels have diminished pulmonary pathology. (A-C) Representative lung sections of HbS/FIIWT mice (left panels) compared with that of HbS/FIIlox/− mice (right panels) showing: (A) increased inflammatory infiltrate in HbS/FIIWT lungs compared with HbS/FIIlox/− lungs. Objective, ×10. (B) Increased alveolar macrophages in HbS/FIIWT lungs compared with HbS/FIIlox/− lungs. Objective, ×40. (C) Increased edema around blood vessels in HbS/FIIWT lungs vs its lack in HbS/FIIlox/− lungs. Objective, ×40. Black arrows indicate the pathology described in each panel. Images are representative of 6 to 9 mice per experimental group. Mice used as transplant recipients were of similar ages (8-10 weeks) with equal numbers of males and females distributed among the experimental groups. Fully chimeric sickle or normal mice were followed for a year posttransplantation.

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