Tumor Xenografts of Human Clear Cell Renal Cell Carcinoma But Not Corresponding Cell Lines Recapitulate Clinical Response to Sunitinib: Feasibility of Using Biopsy Samples

Dong, Yiyu; Manley, Brandon; Becerra, Maria F.; Redzematovic, Almedina; Casuscelli, Jozefina; Tennenbaum, Daniel M.; Reznik, Ed; Han, Song Iy; Benfante, Nicole; Chen, Ying-Bei; Arcila, Maria E.; Aras, Ömer; Voss, Martin H.; Feldman, Darren R.; Motzer, Robert J.; Fabbri, Nicola; Healey, John H.; Boland, Patrick J.; Chawla, Mohit; Durack, Jeremy C.; Lee, Chung-Han; Coleman, Jonathan; Russo, Paul; Hakimi, A. Ari; Cheng, Emily H.; Hsieh, James J.

doi:10.1016/j.euf.2016.08.005

Cited by 33 publications

(31 citation statements)

References 29 publications

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“…We have complied with all relevant ethical regulations. All surgical specimens were transported in RPMI medium or PBS on ice, washed with cold PBS, cut into small pieces (2 × 2 to 3 × 3 mm 3 ) and then implanted subcutaneously into one or two sides of the flank of 6-8-week-old male immunocompromised NOD-SCID IL2Rg −/− (NSG) mice (Jackson Laboratory) via a 4-5 mm skin incision over the mid-lumbar spine 46,47 . PDX from UCC11 was generated from a frozen cell pellet after a collagenbased digestion process.…”

Section: Methodsmentioning

confidence: 99%

Modeling biological and genetic diversity in upper tract urothelial carcinoma with patient derived xenografts

Kim

Audenet

et al. 2020

Nat Commun

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Treatment paradigms for patients with upper tract urothelial carcinoma (UTUC) are typically extrapolated from studies of bladder cancer despite their distinct clinical and molecular characteristics. The advancement of UTUC research is hampered by the lack of diseasespecific models. Here, we report the establishment of patient derived xenograft (PDX) and cell line models that reflect the genomic and biological heterogeneity of the human disease. Models demonstrate high genomic concordance with the corresponding patient tumors, with invasive tumors more likely to successfully engraft. Treatment of PDX models with chemotherapy recapitulates responses observed in patients. Analysis of a HER2 S310F-mutant PDX suggests that an antibody drug conjugate targeting HER2 would have superior efficacy versus selective HER2 kinase inhibitors. In sum, the biological and phenotypic concordance between patient and PDXs suggest that these models could facilitate studies of intrinsic and acquired resistance and the development of personalized medicine strategies for UTUC patients.

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Section: Methodsmentioning

confidence: 99%

Modeling biological and genetic diversity in upper tract urothelial carcinoma with patient derived xenografts

Kim

Audenet

et al. 2020

Nat Commun

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“…Various agents have been tested in the pre-clinical setting using PDX models to investigate tumor response. Importantly, it has been shown that PDX models for RCC can better correlate with clinical response to sunitinib than cancer cell lines [57]. In one of the largest studies to date, Sivavand et al performed validation of targeted therapies in 94 different RCC patient tumor samples, 35 of which yielded viable tumor xenografts, and 16 were able to be serially passed successfully.…”

Section: Correlation With Therapy Response and Chemosensitivitymentioning

confidence: 99%

Patient-Derived Xenograft Models in Urological Malignancies: Urothelial Cell Carcinoma and Renal Cell Carcinoma

Tracey

Murray

Coleman

et al. 2020

Cancers

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The engraftment of human tumor tissues into immunodeficient host mice to generate patient-derived xenograft (PDX) models has become increasingly utilized for many types of cancers. By capturing the unique genomic and molecular properties of the parental tumor, PDX models enable analysis of patient-specific clinical responses. PDX models are an important platform to address the contribution of inter-tumoral heterogeneity to therapeutic sensitivity, tumor evolution, and the mechanisms of treatment resistance. With the increasingly important role played by targeted therapies in urological malignancies, the establishment of representative PDX models can contribute to improved facilitation and adoption of precision medicine. In this review of the evolving role of the PDX in urothelial cancer and kidney cancer, we discuss the essential elements of successful graft development, effective translational application, and future directions for clinical models.

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“…Functional studies based on model systems to recapitulate genetic and phenotypic characteristics of the patient profile such as patient‐derived xenograft (PDX)/tissue grafts (TG), organoids and patient‐derived cultures that have recently been established from RCC . TG models were generally well‐characterized based on histology, gene expression and genomics, and are known to retain regional ITH .…”

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confidence: 99%

“…TG models were generally well‐characterized based on histology, gene expression and genomics, and are known to retain regional ITH . TG models only allow for small scale drug testing studies, however, may recapitulate the drug responsiveness in patients . A study on a single patient's PDX models derived from a primary and a lung metastatic sample showed noticeable variation in drug response profiles inferred from the single cell RNA‐sequencing (scRNA‐seq) of the paired samples, and underlined the impact of ITH in RCC .…”

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confidence: 99%

Clonal heterogeneity influences drug responsiveness in renal cancer assessed by ex vivo drug testing of multiple patient‐derived cancer cells

Saeed

Ojamies

Pellinen

et al. 2018

Intl Journal of Cancer

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Renal cell cancer (RCC) has become a prototype example of the extensive intratumor heterogeneity and clonal evolution of human cancers. However, there is little direct evidence on how the genetic heterogeneity impacts on drug response profiles of the cancer cells. Our goal was to determine how genomic clonal evolution impacts drug responses. Finding from our study could help to define the challenge that clonal evolution poses on cancer therapy. We established multiple patient-derived cells (PDCs) from different tumor regions of four RCC patients, verified their clonal relationship to each other and to the uncultured tumor tissue by genome sequencing. Furthermore, comprehensive drug-sensitivity testing with 460 oncological drugs was performed on all PDC clones. The PDCs retained many cancer-specific copy number alterations and mutations in driver genes such as VHL, PBRM1, PIK3C2A, KMD5C and TSC2 genes. The drug testing highlighted vulnerability in the PDCs toward approved RCC drugs, such as the mTOR-inhibitor temsirolimus, but also novel sensitivities were uncovered. The individual PDC clones from different tumor regions in a patient showed distinct drug-response profiles, suggesting that genomic heterogeneity contributes to the variability in drug responses. Studies of multiple PDCs from a patient with cancer are informative for elucidating cancer heterogeneity and for the determination on how the genomic evolution is manifested in cancer drug responsiveness. This approach could facilitate tailoring of drugs and drug combinations to individual patients.

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Tumor Xenografts of Human Clear Cell Renal Cell Carcinoma But Not Corresponding Cell Lines Recapitulate Clinical Response to Sunitinib: Feasibility of Using Biopsy Samples

Cited by 33 publications

References 29 publications

Modeling biological and genetic diversity in upper tract urothelial carcinoma with patient derived xenografts

Modeling biological and genetic diversity in upper tract urothelial carcinoma with patient derived xenografts

Patient-Derived Xenograft Models in Urological Malignancies: Urothelial Cell Carcinoma and Renal Cell Carcinoma

Clonal heterogeneity influences drug responsiveness in renal cancer assessed by ex vivo drug testing of multiple patient‐derived cancer cells

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