PO.TB05.02 · 肿瘤生物学

Differential sensitivity of paired FUS-TFCP2+ RMS PDX models developed from tumor specimens obtained prior to and after ALK inhibitor therapy

海报缩略图:Differential sensitivity of paired FUS-TFCP2+ RMS PDX models developed from tumor specimens obtained prior to and after ALK inhibitor therapy
编号 6179 展板 15 时间 4/21 02:00–05:00 区域 Section 30 主讲 Erika Dobrota, BS
分会场 Pediatric Cancer Models
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作者与单位

Erika Dobrota1, M. Reza Saadatzadeh1, Barbara Bailey1, Keiko Kreklau1, Gabe Mervis1, Kathy Coy2, Felicia Kennedy2, Melissa Trowbridge2, Anthony Sinn2, Christopher Davis1, Steven Angus1, Michael Ferguson3, Pankita Pandya4, Karen Pollok4

1Wells Center for Pediatric Research, Indiana University School of Medicine, Indianapolis, IN,2Preclinical Modeling and Therapeutics Core, Indiana University Simon Comprehensive Cancer Center, Indianapolis, IN,3Department of Pediatrics, Division of Pediatric Hematology/Oncology, University of Louisville, Louisville, KY,4Indiana University Simon Comprehensive Cancer Center, Indianapolis, IN

摘要 Abstract

FUS-TFCP2-positive rhabdomyosarcoma (FUS-TFCP2+ RMS) is a rare subtype of spindle cell/sclerosing RMS with a craniofacial predilection. These tumors are highly aggressive, quick to metastasize and evade conventional chemotherapies. FUS-TFCP2 fusion results in a gain of function transcription factor that promotes proliferation and activates survival pathways while blocking myogenic differentiation and inhibiting DNA repair. Currently, there is no effective standard of care, surgery can be difficult due to location and patients typically succumb to the disease within 15 months of diagnosis. Overexpression of downstream target, Anaplastic Lymphoma Kinase (ALK), is characteristic of FUS-TFCP2+ RMS. However, while case reports of targeted treatment with ALK inhibitors (ALKi) have shown modest results, resistance always emerges. In collaboration with the Pediatric Cancer Precision Genomics Program at the Riley Hospital for Children, we developed a paired set of FUS-TFCP2+ RMS patient-derived xenografts (PDXs). ALKi-sensitive PDX174 was derived from a patient tumor sample obtained prior to an 11-month ALKi (lorlatinib) regimen. Subsequently, a second sample was acquired following disease progression from which ALKi-resistant PDX199 was established. RT-PCR validated the fusion site in both models. In vivo studies confirmed PDX174 sensitivity and PDX199 resistance to lorlatinib (0.1mg/kg and 1mg/kg). Concordant with FUS-TFCP2+ characterization, transcriptome analysis showed significantly increased expression of ALK in both PDX174 (14.9-fold) and PDX199 (11.1-fold). Western blot analysis revealed robust overexpression of ALK isoforms in PDX174, whereas ALK expression in the ALKi-resistant PDX199 was only barely detectable. Instead, PDX199 exhibited increased levels of TERT, CDK4/6, and BET proteins. To further compare the models, we utilized two complementary approaches to evaluate the activated kinome of ALKi-resistant PDX199 compared to ALKi-sensitive PDX174. Kinase activity profiling using PamGene peptide microarrays revealed a statistically significant increase in kinase activity of components involved in PI3K/AKT pathway and cell cycle CDKs (CDK1,2,4), with concomitant suppression of kinase activity of JNK/p38 MAPKs, indicating a shift toward PI3K/mTOR-driven pro-survival signaling and potential vulnerability to PI3K/AKT and CDK inhibition. Global kinome analysis using multiplexed inhibitor beads also showed an increase in CDK4/6 activation in ALKi-resistant PDX199 versus ALKi-sensitive PDX174. Pre-clinical models such as these provide a platform to connect molecular signatures with targeted therapy, increase our mechanistic understanding of tumor adaptive responses and design therapies that will mitigate the emergence of therapeutic resistance.
利益披露 Disclosure
E. Dobrota, None.. M. R. Saadatzadeh, None.. B. Bailey, None.. K. Kreklau, None.. G. Mervis, None.. K. Coy, None.. F. Kennedy, None.. M. Trowbridge, None.. A. Sinn, None.. C. Davis, None.. S. Angus, None.. M. Ferguson, None.. P. Pandya, None.. K. Pollok, None.

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