Figure 7.
Figure 7. Amelioration of inflammatory response, down-regulation of the UPR effectors, and improvement of neuromotor abilities of Glb1-/- mice after BMT. (A) Immunolabeling using an anti-SDF-1β antibody demonstrated that the level of this chemokine was lower in the thalamus of 6-month-old treated Glb1-/- mice (Glb1-/- BMTβ-gal) than in Glb1-/- mice that underwent mock transplantation (Glb1-/- BMTGFP). Anti-GFAP staining demonstrated attenuation of reactive gliosis in the thalamus of 4-month-old treated Glb1-/- mice. Immunolabeling with anti-F4/80 antibody showed that the proliferation and activation of microglia in the thalamus of 3-month-old treated Glb1-/- mice were reverted to a resting state. Size bar corresponds to 50 μm. (B-C) CHOP and caspase-12 mRNA levels in the hindbrain, midbrain, and forebrain (HMF), brain stem (BS), cerebellum (CB), and spinal cord of treated Glb1-/- mice (▪) were restored to levels that were comparable with those seen in wild-type tissues (▦). (D) Glb1-/- mice that underwent transplantation (▪) performed better than untreated Glb1-/- mice (▦) but not as well as wild-type mice (□) on the rotating rod test of motor coordination and balance (n = 15). (E) Similar results were seen on the open-field exploratory activity test (n = 17). Data are expressed as mean ± SD; groups were compared by one-way repeated measures ANOVA. #P < .05 relative to untreated Glb1-/- littermates at the same age; post hoc Tukey test.

Amelioration of inflammatory response, down-regulation of the UPR effectors, and improvement of neuromotor abilities of Glb1-/- mice after BMT. (A) Immunolabeling using an anti-SDF-1β antibody demonstrated that the level of this chemokine was lower in the thalamus of 6-month-old treated Glb1-/- mice (Glb1-/- BMTβ-gal) than in Glb1-/- mice that underwent mock transplantation (Glb1-/- BMTGFP). Anti-GFAP staining demonstrated attenuation of reactive gliosis in the thalamus of 4-month-old treated Glb1-/- mice. Immunolabeling with anti-F4/80 antibody showed that the proliferation and activation of microglia in the thalamus of 3-month-old treated Glb1-/- mice were reverted to a resting state. Size bar corresponds to 50 μm. (B-C) CHOP and caspase-12 mRNA levels in the hindbrain, midbrain, and forebrain (HMF), brain stem (BS), cerebellum (CB), and spinal cord of treated Glb1-/- mice (▪) were restored to levels that were comparable with those seen in wild-type tissues (▦). (D) Glb1-/- mice that underwent transplantation (▪) performed better than untreated Glb1-/- mice (▦) but not as well as wild-type mice (□) on the rotating rod test of motor coordination and balance (n = 15). (E) Similar results were seen on the open-field exploratory activity test (n = 17). Data are expressed as mean ± SD; groups were compared by one-way repeated measures ANOVA. #P < .05 relative to untreated Glb1-/- littermates at the same age; post hoc Tukey test.

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