Modeling Spontaneous Bone Metastasis Formation of Solid Human Tumor Xenografts in Mice

Labitzky, Vera; Baranowsky, Anke; Maar, Hanna; Hanika, Sandra; Starzonek, Sarah; Ahlers, Ann-Kristin; Stübke, Katrin; Koziolek, Eva Jolanthe; Heine, Markus; Schäfer, Paula; Windhorst, Sabine; Jücker, Manfred; Riecken, Kristoffer; Amling, Michael; Schinke, Thorsten; Schumacher, Udo; Valentiner, Ursula; Lange, Tobias

doi:10.3390/cancers12020385

Cited by 16 publications

(14 citation statements)

References 38 publications

(51 reference statements)

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“…This finding implies that CHD1 suppresses metastatic outgrowth. Metastasis to other sites such as bone marrow can only rarely be found at a very low level in spontaneous metastasis xenografts and requires several modifications of the methodology [26]. As of yet, potential effects of the CHD1 loss on bone metastasis were therefore not determined, which is a limitation of this study.…”

Section: Discussionmentioning

confidence: 97%

CHD1 loss negatively influences metastasis-free survival in R0-resected prostate cancer patients and promotes spontaneous metastasis in vivo

et al. 2021

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The outcome of prostate cancer (PCa) patients is highly variable and depends on whether or not distant metastases occur. Multiple chromosomal deletions have been linked to early tumor marker PSA recurrence (biochemical relapse, BCR) after radical prostatectomy (RP), but their potential role for distant metastasis formation is largely unknown. Here, we specifically analyzed whether deletion of the tumor suppressor CHD1 (5q21) influences the post-surgical risk of distant metastasis and whether CHD1 loss directly contributes to metastasis formation in vivo. By considering >6800 patients we found that the CHD1 deletion negatively influences metastasis-free survival in R0 patients (HR: 2.32; 95% CI: 1.61, 3.33; p < 0.001) independent of preoperative PSA, pT stage, pN status, Gleason Score, and BCR. Moreover, CHD1 deletion predicts shortened BCR-free survival in pT2 patients and cancer-specific survival in all patients. In vivo, CHD1 loss increases spontaneous pulmonary metastasis formation in two distinct PCa models coupled with a higher number of multicellular colonies as compared to single-cell metastases. Transcriptome analyses revealed down-regulation of the PCa-specific metastasis suppressor and TGFβ signaling regulator PMEPA1 after CHD1 depletion in both tested PCa models. CHD1 loss increases the risk of postoperative metastasis in R0-resected PCa patients and promotes spontaneous metastasis formation in vivo.

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Section: Discussionmentioning

confidence: 97%

CHD1 loss negatively influences metastasis-free survival in R0-resected prostate cancer patients and promotes spontaneous metastasis in vivo

et al. 2021

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“…To further investigate the role of ALDH genes in metastasis, we measured the expression of ALDH1A1 and ALDH1A3 genes in the PC3 cells originating from different metastatic sites (Labitzky et al, 2020). Briefly, PC3 cells were first subcutaneously injected into immunodeficient NSG mice, and small pieces of surgically excised xenograft tumors (PT), as well as spontaneous lung (L) and bone marrow (BM) metastases were used for in vitro propagation of sublines PC3-PT, PC3-L, and PC-BM, respectively (Fig.…”

Section: Aldh Genes Differentially Regulate Prostate Cancer Metastasismentioning

confidence: 99%

The distinct role of ALDH1A1 and ALDH1A3 in the regulation of prostate cancer metastases

Gorodetska

Offermann

Pueschel

et al. 2021

Preprint

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Cancer stem cells (CSC) are characterized by high self-renewal capacity, tumor-initiating potential, and therapy resistance. Aldehyde dehydrogenase (ALDH)+ cell population serves as an indicator of prostate CSCs with increased therapy resistance, enhanced DNA double-strand break repair, and activated epithelial-mesenchymal transition (EMT) and migration. Numerous ALDH genes contribute to ALDH enzymatic activity; however, only some of them showed clinical relevance. We found that ALDH1A1 and ALDH1A3 genes functionally regulate CSC properties and radiation sensitivity of PCa. We revealed a negative correlation between ALDH1A1 and ALDH1A3 expression in publicly available prostate cancer (PCa) datasets and demonstrated that ALDH1A1 and ALDH1A3 have opposing predictive value for biochemical recurrence-free survival. Our data suggest an association of ALDH1A1 with the metastatic burden, elucidating the role of ALDH genes in the metastatic spread and homing to the bone, which can be, at least partially, attributed to regulating the transforming growth factor beta 1 (TGFB1) and matrix metalloproteinases (MMPs). ALDH genes play a diverse role in PCa development under AR and β-catenin-dependent regulation, with ALDH1A1 becoming dominant in later stages of tumor development when PCa cells gain androgen independence. Taken together, our results indicate that ALDH1A1 and ALDH1A3 modulate PCa radiosensitivity, regulate CSCs phenotype, and spread of PCa cells to the bone, therefore having clinical implication for identifying patients at high risk for progression to metastatic disease.

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“…Here, we present data comparing the most widely used immunocompetent murine models and their ability to model human NB disease. However, xenograph models, using human tissue or cell lines are another model which can be utilized 15 , 36 , 53 – 56 . Until recently these models mainly used immunompromised mice and therefore it would be difficult to study tumor immunology and immunotherapeutics.…”

Section: Discussionmentioning

confidence: 99%

Immune characterization of pre-clinical murine models of neuroblastoma

Webb

Lanati

Wareham

et al. 2020

Sci Rep

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Immunotherapy offers a potentially less toxic, more tumor-specific treatment for neuroblastoma than conventional cytotoxic therapies. Accurate and reproducible immune competent preclinical models are key to understanding mechanisms of action, interactions with other therapies and mechanisms of resistance to immunotherapy. Here we characterized the tumor and splenic microenvironment of two syngeneic subcutaneous (NXS2 and 9464D), and a spontaneous transgenic (TH-MYCN) murine model of neuroblastoma, comparing histological features and immune infiltrates to previously published data on human neuroblastoma. Histological sections of frozen tissues were stained by immunohistochemistry and immunofluorescence for immune cell markers and tumor architecture. Tissues were dissociated by enzymatic digestion, stained with panels of antibodies to detect and quantify cancer cells, along with lymphocytic and myeloid infiltration by flow cytometry. Finally, we tested TH-MYCN mice as a feasible model for immunotherapy, using prior treatment with cyclophosphamide to create a therapeutic window of minimal residual disease to favor host immune development. Immune infiltration differed significantly between all the models. TH-MYCN tumors were found to resemble immune infiltration in human tumors more closely than the subcutaneous models, alongside similar GD2 and MHC class I expression. Finally, TH-MYCN transgenic mice were administered cyclophosphamide alone or in combination with an anti-GD2 or anti-4-1BB monoclonal antibody, which resulted in increase in survival in both combination therapies. The TH-MYCN transgenic mouse is a promising in vivo model for testing immunotherapy compounds and combination therapy in a preclinical setting.

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Modeling Spontaneous Bone Metastasis Formation of Solid Human Tumor Xenografts in Mice

Cited by 16 publications

References 38 publications

CHD1 loss negatively influences metastasis-free survival in R0-resected prostate cancer patients and promotes spontaneous metastasis in vivo

CHD1 loss negatively influences metastasis-free survival in R0-resected prostate cancer patients and promotes spontaneous metastasis in vivo

The distinct role of ALDH1A1 and ALDH1A3 in the regulation of prostate cancer metastases

Immune characterization of pre-clinical murine models of neuroblastoma

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