An immunocompetent mouse model of human glioblastoma

Semenkow, Samantha; Li, Shen; Kahlert, Ulf D.; Raabe, Eric H.; Xu, Jiadi; Arnold, Antje; Janowski, Mirosław; Oh, Byoung Chol; Brandacher, Gerald; Bulte, Jeff W.M.; Eberhart, Charles G.; Walczak, Piotr

doi:10.18632/oncotarget.17851

Cited by 33 publications

(30 citation statements)

References 46 publications

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“…However, the number of intact breast cancer cells was dramatically reduced after 5 days, although we could still detect isolated DsRed-positive cells and punctate acellular DsRed fluorescence at the lesion site at the end of the experiment. This rapid clearance of the tumour cells may reflect, in part, a graft versus host immune response to the xenotransplantation of a human breast cancer cell line into an immunocompetent mouse [51], although there was very limited infiltration of CD45 hi immune cells at the lesion site. An alternative possibility is that the DsRed cells rapidly die by necrosis or apoptosis, although the significant disruption to the local architecture of the cortical parenchyma in the presence of the cancer cells would argue against this.…”

Section: Discussionmentioning

confidence: 99%

Metastatic breast cancer cells induce altered microglial morphology and electrical excitability in vivo

Simon

Yang

Marrison

et al. 2020

J Neuroinflammation

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Background: An emerging problem in the treatment of breast cancer is the increasing incidence of metastases to the brain. Metastatic brain tumours are incurable and can cause epileptic seizures and cognitive impairment, so better understanding of this niche, and the cellular mechanisms, is urgently required. Microglia are the resident brain macrophage population, becoming "activated" by neuronal injury, eliciting an inflammatory response. Microglia promote proliferation, angiogenesis and invasion in brain tumours and metastases. However, the mechanisms underlying microglial involvement appear complex and better models are required to improve understanding of function. Methods: Here, we sought to address this need by developing a model to study metastatic breast cancer cellmicroglial interactions using intravital imaging combined with ex vivo electrophysiology. We implanted an optical window on the parietal bone to facilitate observation of cellular behaviour in situ in the outer cortex of heterozygous Cx3cr1 GFP/+ mice. Results: We detected GFP-expressing microglia in Cx3cr1 GFP/+ mice up to 350 μm below the window without significant loss of resolution. When DsRed-expressing metastatic MDA-MB-231 breast cancer cells were implanted in Matrigel under the optical window, significant accumulation of activated microglia around invading tumour cells could be observed. This inflammatory response resulted in significant cortical disorganisation and aberrant spontaneously-occurring local field potential spike events around the metastatic site. Conclusions: These data suggest that peritumoral microglial activation and accumulation may play a critical role in local tissue changes underpinning aberrant cortical activity, which offers a possible mechanism for the disrupted cognitive performance and seizures seen in patients with metastatic breast cancer.

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Section: Discussionmentioning

confidence: 99%

Metastatic breast cancer cells induce altered microglial morphology and electrical excitability in vivo

Simon

Yang

Marrison

et al. 2020

J Neuroinflammation

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“…This is highly significant as it allows studying behavior of human cells in various available transgenic mouse models or disease systems where adaptive immunity plays important role such as stroke or multiple sclerosis. We have recently shown that similar strategy with CoB can be used for modeling F o r P e e r R e v i e w human glioblastoma in immunocompetent mice (Semenkow et al, 2017) further demonstrating universal utility of this method.…”

Section: Costimulation Blockade-protected Allogeneic Grps Myelinate Amentioning

confidence: 93%

Induction of immunological tolerance to myelinogenic glial-restricted progenitor allografts

Chu

et al. 2019

Brain

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“…The novel gene editing technology CRISPR-Cas9 could also be applied for the development of humanized mice models by substitute part of the mouse gene with a particular gene of human origin to express functional components of the human immune system [ 90 ], such as PD-1/PD-L1, thus enabling the testing of some immune-targeting agents. Instead of constructing murine models with intact human immune systems, some studies have reported their success in generating xenograft models by transplanting human tumor cell lines into immunosuppressed or immunotolerant mice to construct xenografts with intact murine immune systems [ 91 , 92 ]. Using this approach to establish immunocompetent PDX models may be a promising strategy to optimize current immunodeficient models.…”

Section: Future Perspectivesmentioning

confidence: 99%

Patient-derived xenograft models in musculoskeletal malignancies

Lü

Chen

et al. 2018

J Transl Med

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Successful oncological drug development for bone and soft tissue sarcoma is grossly stagnating. A major obstacle in this process is the lack of appropriate animal models recapitulating the complexity and heterogeneity of musculoskeletal malignancies, resulting in poor efficiency in translating the findings of basic research to clinical applications. In recent years, patient-derived xenograft (PDX) models generated by directly engrafting patient-derived tumor fragments into immunocompromised mice have recaptured the attention of many researchers due to their properties of retaining the principle histopathology, biological behaviors, and molecular and genetic characteristics of the original tumor, showing promising future in both basic and clinical studies of bone and soft tissue sarcoma. Despite several limitations including low take rate and long take time in PDX generation, deficient immune system and heterologous tumor microenvironment of the host, PDXs offer a more advantageous platform for preclinical drug screening, biomarker identification and clinical therapeutic decision guiding. Here, we provide a timely review of the establishment and applications of PDX models for musculoskeletal malignancies and discuss current challenges and future directions of this approach.

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An immunocompetent mouse model of human glioblastoma

Cited by 33 publications

References 46 publications

Metastatic breast cancer cells induce altered microglial morphology and electrical excitability in vivo

Metastatic breast cancer cells induce altered microglial morphology and electrical excitability in vivo

Induction of immunological tolerance to myelinogenic glial-restricted progenitor allografts

Patient-derived xenograft models in musculoskeletal malignancies

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