Figure 1
Figure 1. Characterization of the TRP-1 CD4+ model. (A) Characteristic cappuccino phenotype of white-based brown mutation (Bw) after 8 rounds of backcrossing onto a C57BL/6 background using “speed congenics.” The coat color appearance derives from a defect in exon 1 of tyrosinase-related protein-1 (tyrp1) gene. The MHC class II–restricted TCR used to create the TRP-1–specific transgenic mouse was isolated from Bw mice after multiple rounds of vaccination. (B) RAG1−/−Bw TRP-1 Tg+ animals are marginally protected against the B16 challenge. C57BL/6, RAG1−/−, RAG1−/−Bw, and their RAG1−/−BwTRP-1 TCR transgenic littermates were injected subcutaneously with 0.5 × 106 B16 melanoma cells. Results for tumor area are the mean of measurements from at least 5 mice per group (± SEM). Data shown are representative of 2 independent experiments. (C) Adoptive transfer of 0.25 × 106 naive purified TRP-1 CD4+ T cells into a tyrp1+/+ (wt, black) RAG1−/− mouse results in a rapid development of massive vitiligo. (D) H&E staining of ocular tissue from the mice that received adoptive transfer of naive TRP-1 cells revealed diffuse damage with edema, retinal folding, disruption of pigmented epithelium, and inflammatory infiltrate in the choroid. (E) An H&E stain of a normal eye at a similar magnification from an untreated RAG1−/− mouse is shown as a control.

Characterization of the TRP-1 CD4+ model. (A) Characteristic cappuccino phenotype of white-based brown mutation (Bw) after 8 rounds of backcrossing onto a C57BL/6 background using “speed congenics.” The coat color appearance derives from a defect in exon 1 of tyrosinase-related protein-1 (tyrp1) gene. The MHC class II–restricted TCR used to create the TRP-1–specific transgenic mouse was isolated from Bw mice after multiple rounds of vaccination. (B) RAG1−/−Bw TRP-1 Tg+ animals are marginally protected against the B16 challenge. C57BL/6, RAG1−/−, RAG1−/−Bw, and their RAG1−/−BwTRP-1 TCR transgenic littermates were injected subcutaneously with 0.5 × 106 B16 melanoma cells. Results for tumor area are the mean of measurements from at least 5 mice per group (± SEM). Data shown are representative of 2 independent experiments. (C) Adoptive transfer of 0.25 × 106 naive purified TRP-1 CD4+ T cells into a tyrp1+/+ (wt, black) RAG1−/− mouse results in a rapid development of massive vitiligo. (D) H&E staining of ocular tissue from the mice that received adoptive transfer of naive TRP-1 cells revealed diffuse damage with edema, retinal folding, disruption of pigmented epithelium, and inflammatory infiltrate in the choroid. (E) An H&E stain of a normal eye at a similar magnification from an untreated RAG1−/− mouse is shown as a control.

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