![BCMA-SLAMF7- or BCMA-FAP-CART cells show a long-term durable response and improve overall survival in the MM-TME mouse model. (A-B) Four weeks after the injection of 1 × 106 OPM-2 and 1 × 106 BM-CAFs, mice were randomized into 4 groups: (1) UTD, (2) BCMA-CART cells, (3) BCMA-SLAMF7-CART cells, or (4) BCMA-FAP-CART cells. Tumor burden was assessed by using BLI (4 mice per group). (C) BLI curves of the MM-TME mouse models treated with UTD, single BCMA-CART-, dual-targeted BCMA-SLAMF7-, or BCMA-FAP-CART cells (mean and standard error of the mean; *P < .05, two-way analysis of variance at day 14). (D) Kaplan-Meier survival curves of the MM-TME mouse models treated with UTD, single BCMA-CART-, dual-targeted BCMA-SLAMF7-, or BCMA-FAP-CART cells (BCMA-CART- vs BCMA-SLAMF7-CART cells hazard ratio, 0.03020 [95% confidence interval, 0.001835-0.4969; *P = .01]; BCMA-CART- vs BCMA-FAP-CART cells hazard ratio, 0.03020 [95% confidence interval, 0.001835-0.4969; *P = .01]). (E-F) Mice were bled on day 10 after T-cell infusion. T-cell expansion (E) was analyzed with flow cytometry, and TGF-β levels were analyzed with singleplex (F). Absolute number of T cells per microliter was calculated with counting beads (mean and standard error of the mean; *P < .05, **P < .005, ****P < .0001, one-way analysis of variance). (G) Immunohistochemical analysis of BM samples from MM-TME mice treated with CART cells targeting BCMA, BCMA-SLAMF7, or BCMA-FAP (upper left, upper middle, lower left, and lower middle, magnification ×40; upper right and lower right, magnification ×20). n.s., not significant.](https://ash.silverchair-cdn.com/ash/content_public/journal/blood/139/26/10.1182_blood.2021012811/4/bloodbld2021012811f5.png?Expires=1724941454&Signature=jgzO8VRNKqOTo2UmYP5vUkrTGGoTXXlQ3mrsxX0y4ayGF-BObc5N1j0t9gBstkbBJ-kGOtbORRAEXbunsU1HJPHH47exJda40UJ5WgpAHaXMmvcuRb3yEQQWvPcqNkbH8wQ2TsFwAJC88m9rhClAjId-wG7x3~1ea8d6DjQMiR4ePqRdIzsdSsWFfkgjXk~HvYymajk8cr~D6M4KHpA3RkPVCZXhFG23xd9Ol4WOh~jH6Ydfq0EeCZDQy7Scc1rMdHHXPgFjJSxD-dEIuempvdjlzCwKi62UCsp22VJ2cJF~jy8zVOIDh35owewaGuaok0Eo9gBoRTQxvRNxejIlaA__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
BCMA-SLAMF7- or BCMA-FAP-CART cells show a long-term durable response and improve overall survival in the MM-TME mouse model. (A-B) Four weeks after the injection of 1 × 106 OPM-2 and 1 × 106 BM-CAFs, mice were randomized into 4 groups: (1) UTD, (2) BCMA-CART cells, (3) BCMA-SLAMF7-CART cells, or (4) BCMA-FAP-CART cells. Tumor burden was assessed by using BLI (4 mice per group). (C) BLI curves of the MM-TME mouse models treated with UTD, single BCMA-CART-, dual-targeted BCMA-SLAMF7-, or BCMA-FAP-CART cells (mean and standard error of the mean; *P < .05, two-way analysis of variance at day 14). (D) Kaplan-Meier survival curves of the MM-TME mouse models treated with UTD, single BCMA-CART-, dual-targeted BCMA-SLAMF7-, or BCMA-FAP-CART cells (BCMA-CART- vs BCMA-SLAMF7-CART cells hazard ratio, 0.03020 [95% confidence interval, 0.001835-0.4969; *P = .01]; BCMA-CART- vs BCMA-FAP-CART cells hazard ratio, 0.03020 [95% confidence interval, 0.001835-0.4969; *P = .01]). (E-F) Mice were bled on day 10 after T-cell infusion. T-cell expansion (E) was analyzed with flow cytometry, and TGF-β levels were analyzed with singleplex (F). Absolute number of T cells per microliter was calculated with counting beads (mean and standard error of the mean; *P < .05, **P < .005, ****P < .0001, one-way analysis of variance). (G) Immunohistochemical analysis of BM samples from MM-TME mice treated with CART cells targeting BCMA, BCMA-SLAMF7, or BCMA-FAP (upper left, upper middle, lower left, and lower middle, magnification ×40; upper right and lower right, magnification ×20). n.s., not significant.