![Fig. 5. Depletion of alloreactive T cells by AICD prevents acute GvHD in a murine P→F1 GvHD model. / Depicted are survival curves representing 3 independent experiments in which F1 recipients (n = 10) received 2.5 × 106 purified viable parental donor T lymphocytes. T cells from C3H/He mice (H-2k) previously primed to H-2d alloantigen in vivo were restimulated with H-2d–expressing BALB/c stimulator cells and depleted from alloreactivity by AICD. Following adoptive transfer of treated T lymphocytes into irradiated (6.5 Gy [650 cGy]) female F1hosts, recipients did not develop acute GvHD, in contrast to mice injected with untreated allogeneic control cell blasts. (A) Depletion of transferred CD4+ T cells from host reactivity by induction of AICD into F1 recipients prevents development of acute GvHD (▪, P < .05). In contrast, transfer of activated untreated control cells (▾) or donor T lymphocytes depleted of alloreactive responders by soluble anti-CD95 mAb (●) led to rapid and lethal GvHD within 20 days after transfer (P < .05). Controls shown received equivalent numbers of syngeneic spleen cells (■). (B) The same experiments as described in panel A but performed with allogeneic CD8+ T cells are presented.](https://ash.silverchair-cdn.com/ash/content_public/journal/blood/99/8/10.1182_blood.v99.8.3041/5/h80822435005.jpeg?Expires=1726835156&Signature=WtrsjAI7Xp8fjhGxJLDMxTj7UnRthHpfILWo6bjdKCCS0vC3GsAjv9UhU~xLe~6SZg61tcBSlE71SDlbVRvcLSGkZoL8xPv7QTn~dPd4iD63ox0lCt4xln2yM1qATTvBlV-j1CDg7Ht91HDxIxkMjH~9Tqti1fuDFbYlCs3hXv8ZT6rbGXN7XgGN8uYVdsynXD~ZlG2FC1lzNjNVKSOQ4jGb98ljQGXBF-JS2iZUOikJABjzKNSc5yCc5iPk0l6Ljae94jV46PgAdb3AgIbSaSedGwEvMzwa8gPE4fwOcgbQH~kNqFvgXjWDIiVT8dCIoFmvGLEv8CPeXXaUq4rPFw__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
Depletion of alloreactive T cells by AICD prevents acute GvHD in a murine P→F1 GvHD model.
Depicted are survival curves representing 3 independent experiments in which F1 recipients (n = 10) received 2.5 × 106 purified viable parental donor T lymphocytes. T cells from C3H/He mice (H-2k) previously primed to H-2d alloantigen in vivo were restimulated with H-2d–expressing BALB/c stimulator cells and depleted from alloreactivity by AICD. Following adoptive transfer of treated T lymphocytes into irradiated (6.5 Gy [650 cGy]) female F1hosts, recipients did not develop acute GvHD, in contrast to mice injected with untreated allogeneic control cell blasts. (A) Depletion of transferred CD4+ T cells from host reactivity by induction of AICD into F1 recipients prevents development of acute GvHD (▪, P < .05). In contrast, transfer of activated untreated control cells (▾) or donor T lymphocytes depleted of alloreactive responders by soluble anti-CD95 mAb (●) led to rapid and lethal GvHD within 20 days after transfer (P < .05). Controls shown received equivalent numbers of syngeneic spleen cells (■). (B) The same experiments as described in panel A but performed with allogeneic CD8+ T cells are presented.
