Benign tumors in TSC are amenable to treatment by GD3 CAR T cells in mice
Ancy Thomas, Saurav Sumughan, Emilia R. Dellacecca, Rohan S. Shivde, Nicola Lancki, Zhussipbek Mukhatayev, Cristina C. Vaca, Fei Han, Levi Barse, Steven W. Henning, Jesus Zamora-Pineda, Suhail Akhtar, Nikhilesh Gupta, Jasmine O. Zahid, Stephanie R. Zack, Prathyaya Ramesh, Dinesh Jaishankar, Agnes S.Y. Lo, Joel Moss, Maria M. Picken, Thomas N. Darling, Denise M. Scholtens, Daniel F. Dilling, Richard P. Junghans, I. Caroline Le Poole
Ancy Thomas, Saurav Sumughan, Emilia R. Dellacecca, Rohan S. Shivde, Nicola Lancki, Zhussipbek Mukhatayev, Cristina C. Vaca, Fei Han, Levi Barse, Steven W. Henning, Jesus Zamora-Pineda, Suhail Akhtar, Nikhilesh Gupta, Jasmine O. Zahid, Stephanie R. Zack, Prathyaya Ramesh, Dinesh Jaishankar, Agnes S.Y. Lo, Joel Moss, Maria M. Picken, Thomas N. Darling, Denise M. Scholtens, Daniel F. Dilling, Richard P. Junghans, I. Caroline Le Poole
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Research Article Immunology Therapeutics

Benign tumors in TSC are amenable to treatment by GD3 CAR T cells in mice

Abstract

Mutations underlying disease in tuberous sclerosis complex (TSC) give rise to tumors with biallelic mutations in TSC1 or TSC2 and hyperactive mammalian target of rapamycin complex 1 (mTORC1). Benign tumors might exhibit de novo expression of immunogens, targetable by immunotherapy. As tumors may rely on ganglioside D3 (GD3) expression for mTORC1 activation and growth, we compared GD3 expression in tissues from patients with TSC and controls. GD3 was overexpressed in affected tissues from patients with TSC and also in aging Tsc2+/– mice. As GD3 overexpression was not accompanied by marked natural immune responses to the target molecule, we performed preclinical studies with GD3 chimeric antigen receptor (CAR) T cells. Polyfunctional CAR T cells were cytotoxic toward GD3-overexpressing targets. In mice challenged with Tsc2–/– tumor cells, CAR T cells substantially and durably reduced the tumor burden, correlating with increased T cell infiltration. We also treated aged Tsc2+/– heterozygous (>60 weeks) mice that carry spontaneous Tsc2–/– tumors with GD3 CAR or untransduced T cells and evaluated them at endpoint. Following CAR T cell treatment, the majority of mice were tumor free while all control animals carried tumors. The outcomes demonstrate a strong treatment effect and suggest that targeting GD3 can be successful in TSC.

Authors

Ancy Thomas, Saurav Sumughan, Emilia R. Dellacecca, Rohan S. Shivde, Nicola Lancki, Zhussipbek Mukhatayev, Cristina C. Vaca, Fei Han, Levi Barse, Steven W. Henning, Jesus Zamora-Pineda, Suhail Akhtar, Nikhilesh Gupta, Jasmine O. Zahid, Stephanie R. Zack, Prathyaya Ramesh, Dinesh Jaishankar, Agnes S.Y. Lo, Joel Moss, Maria M. Picken, Thomas N. Darling, Denise M. Scholtens, Daniel F. Dilling, Richard P. Junghans, I. Caroline Le Poole

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Figure 3

GD3 CAR T cells respond to antigen in vitro.

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GD3 CAR T cells respond to antigen in vitro. (A) Schematic representatio...
(A) Schematic representation of the GD3 CAR construct used. Fv, variable domain of antibody; TM, transmembrane domain; LTR, long terminal repeat. (B) Efficient transduction of both CD4+ and CD8+ T cells by our second-generation GD3 CAR. (C) IFN-γ secretion by GD3 CAR T cells in response to LB1 Tsc2/ mouse kidney tumor cells. This experiment was performed 3 times with similar results. A representative experiment is shown. Results were analyzed by 2-way ANOVA followed by Bonferroni’s multiple comparisons test. m, murine; E:T, effector/target ratio. (D) Cytotoxicity of GD3 CAR T cells toward LB1 Tsc2–/– mouse kidney tumor cells when cocultured at an E:T ratio of 10:1. A generalized linear mixed model with log link and 0-inflated quasi-Poisson distribution assumption was used and included fixed effects for treatment group and a random effect for wells. Three images/well were acquired every 3 hours for 48 hours, and apoptotic cells stained by caspase-7 red dye were quantified. ****P < 0.0001. (E) Representative images of target cell death (red) induced by GD3 CAR T cells and untransduced T cells, scale bar: 400 μm.