Your search keyword '"Kayembe, Clarisse"' showing total 2 results

1. CAR T cells targeting BAFF-R can overcome CD19 antigen loss in B cell malignancies.

Author

Qin, Hong, Dong, Zhenyuan, Wang, Xiuli, Cheng, Wesley A., Wen, Feng, Xue, Weili, Sun, Han, Walter, Miriam, Wei, Guowei, Smith, D. Lynne, Sun, Xiuhua, Fei, Fan, Xie, Jianming, Panagopoulou, Theano I., Chen, Chun-Wei, Song, Joo Y., Aldoss, Ibrahim, Kayembe, Clarisse, Sarno, Luisa, and Müschen, Markus

Subjects

CD19 antigen, T cells, T cell receptors, B cells, RITUXIMAB, CHIMERIC antigen receptors, LYMPHOBLASTIC leukemia, ACUTE leukemia

Abstract

Circumventing CD19 antigen loss: Chimeric antigen receptor (CAR) T cell treatment for B cell malignancies was pioneered with CD19-targeted CAR T cells. Despite robust clinical responses, relapse due to CD19 antigen loss is common. Qin et al. examined B cell activating factor receptor (BAFF-R) as an alternate CAR T cell target. BAFF-R–targeted CAR T cells could kill multiple human lymphoma and leukemia cell lines, either in vitro or in mice, as well as patient-derived samples. The BAFF-R-CAR T cells could also eradicate tumors lacking CD19. Their compelling preclinical results support the clinical development of BAFF-R–targeted CAR T cells for combating B cell malignancies. CAR T cells targeting CD19 provide promising options for treatment of B cell malignancies. However, tumor relapse from antigen loss can limit efficacy. We developed humanized, second-generation CAR T cells against another B cell–specific marker, B cell activating factor receptor (BAFF-R), which demonstrated cytotoxicity against human lymphoma and acute lymphoblastic leukemia (ALL) lines. Adoptively transferred BAFF-R-CAR T cells eradicated 10-day preestablished tumor xenografts after a single treatment and retained efficacy against xenografts deficient in CD19 expression, including CD19-negative variants within a background of CD19-positive lymphoma cells. Four relapsed, primary ALLs with CD19 antigen loss obtained after CD19-directed therapy retained BAFF-R expression and activated BAFF-R-CAR, but not CD19-CAR, T cells. BAFF-R-CAR, but not CD19-CAR, T cells also demonstrated antitumor effects against an additional CD19 antigen loss primary patient–derived xenograft (PDX) in vivo. BAFF-R is amenable to CAR T cell therapy, and its targeting may prevent emergence of CD19 antigen loss variants. [ABSTRACT FROM AUTHOR]

Published

2019

2. A Novel JAK1 Mutant Breast Implant-Associated Anaplastic Large Cell Lymphoma Patient-Derived Xenograft Fostering Pre-Clinical Discoveries.

Author

Fiore, Danilo, Cappelli, Luca Vincenzo, Zumbo, Paul, Phillips, Jude M., Liu, Zhaoqi, Cheng, Shuhua, Yoffe, Liron, Ghione, Paola, Di Maggio, Federica, Dogan, Ahmet, Khodos, Inna, de Stanchina, Elisa, Casano, Joseph, Kayembe, Clarisse, Tam, Wayne, Betel, Doron, Foa', Robin, Cerchietti, Leandro, Rabadan, Raul, and Horwitz, Steven

Subjects

BIOLOGICAL models, BREAST implants, CELL lines, CHROMOSOME abnormalities, DRUG design, CLINICAL drug trials, GENE expression, INTERLEUKINS, GENETIC mutation, RNA, XENOGRAFTS, PHENOTYPES, ANAPLASTIC large-cell lymphoma, SEQUENCE analysis, IN vitro studies, GENOTYPES, JANUS kinases, IN vivo studies, DISEASE risk factors

Abstract

Breast implant-associated lymphoma (BIA-ALCL) has recently been recognized as an independent peripheral T-cell lymphoma (PTCL) entity. In this study, we generated the first BIA-ALCL patient-derived tumor xenograft (PDTX) model (IL89) and a matching continuous cell line (IL89_CL#3488) to discover potential vulnerabilities and druggable targets. We characterized IL89 and IL89_CL#3488, both phenotypically and genotypically, and demonstrated that they closely resemble the matching human primary lymphoma. The tumor content underwent significant enrichment along passages, as confirmed by the increased variant allele frequency (VAF) of mutations. Known aberrations (JAK1 and KMT2C) were identified, together with novel hits, including PDGFB, PDGFRA, and SETBP1. A deep sequencing approach allowed the detection of mutations below the Whole Exome Sequencing (WES) sensitivity threshold, including JAK1G1097D, in the primary sample. RNA sequencing confirmed the expression of a signature of differentially expressed genes in BIA-ALCL. Next, we tested IL89's sensitivity to the JAK inhibitor ruxolitinib and observed a potent anti-tumor effect, both in vitro and in vivo. We also implemented a high-throughput drug screening approach to identify compounds associated with increased responses in the presence of ruxolitinib. In conclusion, these new IL89 BIA-ALCL models closely recapitulate the primary correspondent lymphoma and represent an informative platform for dissecting the molecular features of BIA-ALCL and performing pre-clinical drug discovery studies, fostering the development of new precision medicine approaches. [ABSTRACT FROM AUTHOR]

Published

2020