786-O Xenograft Model - Altogen Labs (2024)

786-O Xenograft Model - Altogen Labs (1)

786-O xenograft model

The most common type of kidney cancer is renal cell carcinoma (RCC), accounting for nearly 3 percent of tumors in adults. The exact cause of renal cell carcinoma is currently unknown. Xenograft rodent models are essential in preclinical studies for testing novel therapeutic modalities to address renal cancer. The 786-O epithelial cell line is isolated from primary adenocarcinoma cells of the kidney tissue of a 58-year-old Caucasian male patient with renal cell adenocarcinoma. 786-O is a hypertriploid cell line that produces parathyroid hormone (PTH) and is tumorigenic in nude mice. 786-O cells display both microvilli and desmosomes. The 786-O cell line is invaluable for studying human infections related to the prostate. 786-O is one of the first RCC cell lines that is commonly used in RCC-focused research. A 2013 renal xenograft study published in British Journal of Cancer, demonstrates that resistance to sunitinib is accompanied by increased COX-2 expression in areas of tumor hypoxia in the 786-O xenograft model. Also, the COX-2 inhibitor celecoxib enhances the effectiveness of sunitinib in the 786-O xenograft model by delaying time to progression if administered early in the course of sunitinib therapy. Celecoxib showed activity in the 786-O tumor model as a single agent and in combination with sunitinib. The 786-O RCC line expresses high levels of VEGF (Vascular endothelial growth factor), which stimulates angiogenesis and gives rise to tumors in nude mice. A 2010 study (Bhatt et al.) used the 786-O model to study the mechanism of resistance that often surfaces within 6-12 months of anti-angiogenesis treatment of metastatic renal cancer. Their results demonstrated that treatment with either sunitinib or sorafenib initially targeted VEGF however resistance was in part due to resumption of angiogenesis correlated to downregulation of IFN-gamma angiostatic chemokines; when the conventional chemotherapies were combined with CXCL9 (one of the angiostatic chemokines) treatment, prolonged reduction of angiogenesis was observed thus providing potential combination clinical strategies for overcoming resistance. Lastly, a 2017 Tumor Biology study used the 786-O model to demonstrate that Rap2B can promote angiogenesis through PI3K/AKT pathway in vivo, and loss of Rap2B could be a novel strategy for RCC anti-angiogenesis therapy. The 786-O cell line (human kidney) is used to create the CDX (Cell Line Derived Xenograft) 786-O xenograft mouse model that allows researchers to study COX-2 inhibitors and anti-angiogenesis therapy as well as anti-cancer agents targeting RCC cells.

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Basic study design

1. 786-O cells are cultured under aseptic conditions in exponential growth phase prior to injection.
2. The cells are trypsinized from the flasks and viable cell counts are determined using a trypan blue exclusion assay (98% cell viability required). The cell suspension is adjusted to the appropriate density.
3. Each mouse (athymic BALB/C or NOD/SCID, 10-12 w.o.) receive a subcutaneous injection in the flank of the hind leg of one million cells in a volume of 100 microliters of Matrigel 786-O cell suspension.
4. The injection sites are manually palpated three times weekly until tumors are established. Tumors are measured using digital calipers until they reach an average size of 50-150 mm3.
5. Animals are randomized into treatment cohorts and administration of the compound of interest is performed according to the treatment schedule.
6. Tumors are measured daily and mouse weights recorded 3 times weekly.
7. Animals are euthanized when tumor size reaches 2,000 sq. millimeters or the IACUC protocol predetermined size limit.
8. Necropsy and tissue collections are performed as defined for termination of experiment.
9. Tumors are excised, weighed and documented by digital imaging.
10. Standard gross necropsies are performed and tissues are collected for downstream analysis.
11. Tumors and tissues aresnap frozen in LN2 and prepared for histology or gene expression analysis.

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Animal handling and maintenance at the Altogen Labs facility is IACUC-regulated and GLP-compliant. Following acclimation to the vivarium environment, mice are sorted according to body mass. The animals are examined daily for tumor appearance and clinical signs. We provide detailed experimental procedures, health reports and data (all-inclusive report is provided to the client that includes methods, results, discussion and raw data along with statistical analysis). Additional services available include collection of tissue, histology, isolation of total protein or RNA and analysis of gene expression.

Following options are available for the 786-O xenograft model:

  • 786-O Tumor Growth Delay (TGD; latency)
  • 786-O Tumor Growth Inhibition (TGI)
  • Dosing frequency and duration of dose administration
  • 786-O tumor immunohistochemistry
  • Blood chemistry analysis
  • Toxicity and survival (optional: performing a broad health observation program)
  • Gross necropsies and histopathology
  • Lipid distribution and metabolic assays
  • Imaging studies

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786-O Xenograft Model - Altogen Labs (2024)

FAQs

What is the xenograft model of cancer? ›

Xenograft models are based on the implantation of human tumor cells into immunocompromised mice to avoid graft versus host reaction of the mouse against the human tumor tissue. Reaction Biology's in vivo tumor models are derived from a variety of origins such as breast, colon, lung, skin, blood.

What is the xenograft model of breast cancer? ›

Breast cancer xenograft models are used to study the biology of breast cancer, including the mechanisms of tumor growth and metastasis, as well as the tumor's response to various treatments types.

What is a subcutaneous xenograft model? ›

Orthotopic xenografts are defined as the implantation of cancer cells into the same organ or tissue from which the cancer originated in the human, while subcutaneous xenografts are the implantation of cancer cells under the skin of an immunodeficient mouse or SRG rat.

Why are xenograft models used? ›

In preclinical research, xenografts are commonly used to test the efficacy of new cancer treatments. Xenograft models are used to study tumor growth and response to test article (novel cancer therapies).

What are the disadvantages of the Xenograft model? ›

One major disadvantage of subcutaneous xenograft tumor models is that the microenvironment of the implanted tumor does not reproduce the environment in which the tumor grows [47][48][49].

What are the risks of Xenograft? ›

Viral Infections after Xenotransplantation

Viral infections carried by transplanted organs may be activated by immunosuppression, inflammation associated with ischemia–reperfusion injury, graft rejection, or reduced antiviral immune responses in major histocompatibility complex–mismatched grafts.

What is the most common xenograft used? ›

A xenograft refers to tissue taken from one species and placed into another species. For intraoral bone replacement grafts, the most common animal sources are bovine and porcine.

Is xenograft permanent or temporary? ›

Allograft and xenograft skin grafts are usually temporary. They cover the damaged skin until the wound heals or the person grows enough healthy skin to use for a permanent skin graft.

What is the medical term for xenograft? ›

xenograft. noun. xe·​no·​graft ˈzen-ə-ˌgraft ˈzēn- : a graft of tissue taken from a donor of one species and grafted into a recipient of another species. called also heterograft, heterotransplant, xenotransplant.

Why do we use xenograft? ›

A xenograft is the transplant of one tissue to another species. Patient-derived xenograft (PDX) is transplanting cancer tissue of one individual to another species and aims to investigate the molecular characteristics, drug response, and the aggressiveness of the tumor formation.

What is a xenograft procedure? ›

Definitions related to xenograft procedure: (xenograft) The transplant of an organ, tissue, or cells to an individual of another species. NCI Dictionary of Cancer Terms. U.S. National Cancer Institute, 2021.

What is the source of Xenograft? ›

Xenografts are bone grafts from other species (typically bovine and porcine) and transplanted in humans. It is osteoconductive, biocompatible and structurally similar to human bone. Plenty of donor sources can found for bone grafting. Bovine, Equine Porcine bones and natural coral are used for xenografting.

What is a tumor xenograft? ›

A tumor xenograft refers to the transplantation of tumor tissue from a patient into a mouse model, allowing for the study of drug efficacy and the retention of tumor characteristics. From: Pathobiology of Human Disease, 2014.

What are the benefits of patient derived xenografts? ›

Patient-Derived Xenografts

Establishing xenograft tumor models from patient-derived tumor tissue at low passage is believed to conserve original tumor characteristics such as tumor architecture, genetic and phenotypic heterogeneity, and sensitivity towards cancer treatment.

What is the success rate of patient derived xenograft? ›

PDX models were considered established after two consecutive passages in mice (P2) and if they passed three validation tests. Of 269 engrafted FNAs, 62 resulted in successful PDX establishment, for an overall take-rate of 23%.

What is allograft vs xenograft model? ›

Allografts are carefully selected and processed human bone materials, while xenografts are derived from animals and possess similar chemical composition to human bone. Synthetic materials such as ceramics and bioactive glasses are used for small defects but may lack osteoinductivity and moldability.

What is an example of a Xenograft? ›

Bone Graft Harvesting

Xenografts are tissues transplanted from one species to another. Xenografts give less consistent results than autograft or allograft, because of histocompatibility differences. Kiel (calf bone) grafts have been used in spine surgery, although their use is of historical significance only.

How does xenograft work? ›

Xenotransplantation is any procedure that involves the transplantation, implantation or infusion into a human recipient of either (a) live cells, tissues, or organs from a nonhuman animal source, or (b) human body fluids, cells, tissues or organs that have had ex vivo contact with live nonhuman animal cells, tissues or ...

What do you mean by xenograft? ›

(ZEE-noh-graft) The transplant of an organ, tissue, or cells to an individual of another species.

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