Oral Mucosal Organoids as a Potential Platform for Personalized Cancer Therapy

Driehuis, Else; Kolders, Sigrid; Spelier, Sacha; Lõhmussaar, Kadi; Willems, Stefan M.; Devriese, Lot A.; Bree, Remco de; Ruiter, Emma J. de; Korving, Jeroen; Begthel, Harry; Es, Johan H. van; Geurts, Veerle; He, Gui Wei; Jaarsveld, Richard H. van; Oka, Rurika; Muraro, Mauro J.; Vivié, Judith; Zandvliet, Maurice M.J.M.; Hendrickx, Antoni P. A.; Iakobachvili, Nino; Sridevi, Priya; Kranenburg, Onno; Boxtel, Ruben van; Kops, Geert J.P.L.; Tuveson, David A.; Peters, Peter J.; Oudenaarden, Alexander van; Clevers, Hans

doi:10.1158/2159-8290.cd-18-1522

Cited by 243 publications

(236 citation statements)

References 80 publications

(80 reference statements)

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“…In the recent past, drug screens have also been reported for PDOs established from many other organs, including liver [40], ovarian [32] and stomach [33] tumours. In addition to drug screens, a recent study of head and neck tumours applied radiation screens in PDOs and compared the results with the clinical outcome [34]. Three patients relapsed after radiotherapy within one to six months, consistent with the finding that their organoid lines were classified as most resistant.…”

Section: In Vitro Culture Systemssupporting

confidence: 58%

“…While these experiments are important to characterize in greater detail the interplay between tumour and immune cells, it needs to be shown to what degree they will add to the predictive value of organoids in clinical set-ups. First trial experiments using organoids for radiation and drug screens showed good correlation with the respective in vivo patient responses [33,34].…”

Section: Clinical Relevance and Implementationmentioning

confidence: 95%

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The potential and challenges of patient-derived organoids in guiding the multimodality treatment of upper gastrointestinal malignancies

et al. 2020

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The incidence of adenocarcinoma at the gastrooesophageal junction increased over the last years. Curative treatment for patients with upper gastrointestinal (UGI) malignancies, such as oesophageal and gastric tumours, is challenging and requires a multidisciplinary approach. Radical surgical resection with complete lymphadenectomy is the cornerstone of UGI cancer treatment. Combined with peri-operative treatment (i.e. by applying CROSS, EOX or FLOT regimen), the survival is even better than with surgery alone. However, peri-operative treatment is not effective in all patients, and the most effective strategy is a topic of active debate, as is reflected by varying treatment guidelines between countries. UGI cancers are (epi)genetically highly heterogeneous. It is thus not likely that a uniform treatment will benefit all patients equally well. Over recent years, patient-derived organoids (PDOs) gained more and more interest as an in vitro prediction model that may assist as a diagnostic tool in the future to select and eventually optimize the best peri-operative treatments for each patient. PDOs can be derived from endoscopic tumour biopsies, which maintain heterogeneity in culture. They can be rapidly established and expanded in a relatively short time for in vitro drug screening experiments. This review summarizes the clinical and molecular aspects of oesophageal and gastric tumours, as well as the current progress and remaining challenges in the use of PDOs for drug and radiation screens.

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Section: In Vitro Culture Systemssupporting

confidence: 58%

Section: Clinical Relevance and Implementationmentioning

confidence: 95%

The potential and challenges of patient-derived organoids in guiding the multimodality treatment of upper gastrointestinal malignancies

et al. 2020

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“…For tubuloid experiments, the drug safety screening was performed using a protocol derived from Driehuis et al 64 . In short, BME was dissolved by incubation in 1 mg/mL dispase II for 30 min at 37…”

Section: Cell Viability Assaysmentioning

confidence: 99%

Cysteamine-bicalutamide combination treatment restores alpha-ketoglutarate and corrects proximal tubule phenotype in cystinosis

Jamalpoor

Gelder

Yengej

et al. 2020

Preprint

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Nephropathic cystinosis is a severe monogenetic kidney disorder caused by mutations in CTNS, encoding the lysosomal transporter cystinosin, resulting in lysosomal cystine accumulation. The sole treatment, cysteamine, slows down the disease progression, but does not correct the established proximal tubulopathy. Here, we developed a new therapeutic strategy by applying an omics-based strategy to expand our knowledge on the complexity of the disease and prioritize drug targets in cystinosis. We identified alpha-ketoglutarate as a key metabolite linking cystinosin loss, lysosomal autophagy defect and proximal tubular impairment in cystinosis. This insight offered a bicalutamide-cysteamine combination treatment as a novel dual target pharmacological approach for the phenotypical correction of cystinotic proximal tubule cells, patient-derived kidney tubuloids and cystinotic zebrafish.

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“…Because the organoids possess many functional and structural characteristics of the original tissue and retain their tumorigenic potential, this technology has now opened completely new perspectives in human research. Organoids generated from individual patients offer the future to study and identify molecular mechanisms in pathophysiology, in transformation and progression of tumor growth, screening and prediction of response and sensitivity to chemotherapeutic drugs, and ultimately the possibility of personalized therapy 6,7 .…”

mentioning

confidence: 99%

Intestinal ex vivo organoid culture reveals altered programmed crypt stem cells in patients with celiac disease

Dieterich

Neurath

Zopf

2020

Sci Rep

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the ex vivo generation of gastrointestinal organoids from crypt stem cells opens up the possibility of new research approaches investigating gastrointestinal diseases. We used this technology to study differences between healthy controls and patients with celiac disease (CD). We noticed distinct dissimilarities in the phenotypes of organoids between our study groups and found considerable variations in their gene expression. Extracellular matrix genes involved in epithelial-mesenchymal transition are expressed most differently. In addition, we demonstrated epigenetic modifications that might be responsible for the different organoid gene expression thus accounting for a deranged crypt/villus axis development in CD. The organoids have proven valuable to demonstrate fundamental differences in duodenal derived organoids between healthy controls and patients with CD and thus are a suitable tool to gain new insights in pathogenesis of CD.

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Oral Mucosal Organoids as a Potential Platform for Personalized Cancer Therapy

Cited by 243 publications

References 80 publications

The potential and challenges of patient-derived organoids in guiding the multimodality treatment of upper gastrointestinal malignancies

The potential and challenges of patient-derived organoids in guiding the multimodality treatment of upper gastrointestinal malignancies

Cysteamine-bicalutamide combination treatment restores alpha-ketoglutarate and corrects proximal tubule phenotype in cystinosis

Intestinal ex vivo organoid culture reveals altered programmed crypt stem cells in patients with celiac disease

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