SUMO pathway inhibition targets an aggressive pancreatic cancer subtype

Biederstädt, Alexander; Hassan, Zonera; Schneeweis, Christian; Schick, Markus; Schneider, Lara; Muckenhuber, Alexander; Hong, Ying-Fen; Siegers, Gerrit; Nilsson, Lisa M.; Wirth, Matthias; Dantes, Zahra; Steiger, Katja; Schunck, Kathrin; Langston, Steve; Lenhof, Hans‐Peter; Coluccio, Andrea; Orben, Felix; Slawska, Jolanta; Scherger, Anna Katharina; Saur, Dieter; Müller, Stefan; Rad, Roland; Weichert, Wilko; Nilsson, Jonas A.; Reichert, Maximilian; Schneider, Günter; Keller, Ulrich

doi:10.1136/gutjnl-2018-317856

Cited by 72 publications

(108 citation statements)

References 59 publications

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“…34 Both ML-792 and ML-93 inhibit the growth of PDAC cells and show a significant correlation in their half-maximal growth inhibitory concentrations in a large panel of murine PDAC cell lines. 22 In sensitive pancreatic cancer models, ML-93 was effective in the double-digit nanomolar range, which was lower than the range observed using ML-792, resulting in the accumulation of cells in the G2/M phase of the cell cycle and in polyploidy with associated apoptosis. 22 These results demonstrate the importance of SUMOylation for proper mitotic progression.…”

Section: Inhibitors Of the Sumo Pathwaymentioning

confidence: 90%

“…22 In sensitive pancreatic cancer models, ML-93 was effective in the double-digit nanomolar range, which was lower than the range observed using ML-792, resulting in the accumulation of cells in the G2/M phase of the cell cycle and in polyploidy with associated apoptosis. 22 These results demonstrate the importance of SUMOylation for proper mitotic progression. 35 An ML-792/ML-93-derived SAE inhibitor, TAK-981, entered clinical development in 2019, with Phase 1 trials recruiting patients with any advanced or metastatic solid tumour and lymphoma (NCT03648372 and NCT04074330).…”

Section: Inhibitors Of the Sumo Pathwaymentioning

confidence: 90%

“…Tissuebased analysis and mRNA expression profiles have defined an aggressive PDAC subtype that shows evidence of hyperactivity of the core SUMO pathway and thereby links the SUMO pathway with less-differentiated PDACs-the basal-like subtype-and an unfavourable prognosis. 22 Mechanistic studies in PDAC link the SUMO pathway in particular with the response towards chemotherapies and to mechanisms of treatment resistance.…”

Section: The Sumo Pathway In Pdacmentioning

confidence: 99%

“…ML-792 and ML-93 form covalent adducts with SUMOs and thereby block SAE and the transfer of SUMOs to the E2 enzyme, UBC9. 22,34 ML-792 and ML-93 in the nanomolar range reduce the fraction of SUMO-bound UBC9 and, consequently total protein SUMOylation, with no crossreactivity with the NEDDylation and ubiquitinylation machineries; 22,34 furthermore, when screened against 366 ATPdependent enzymes, ML-792 demonstrated specificity for the SAE complex. 34 ML-792 induces a failure of mitotic progression and chromosome segregation, with a consequent increase in endoreduplication and polyploidy.…”

Section: Inhibitors Of the Sumo Pathwaymentioning

confidence: 99%

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The SUMO pathway in pancreatic cancer: insights and inhibition

et al. 2020

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An urgent medical need to develop novel treatment strategies for patients with pancreatic ductal adenocarcinoma (PDAC) exists. However, despite various efforts in the histopathological and molecular subtyping of PDAC, novel targeted or specific therapies have not been established. Posttranslational modifications (PTMs) with ubiquitin-like proteins, including small ubiquitin-like modifiers (SUMOs), mediate numerous processes that can contribute to the fitness and survival of cancer cells. The contribution of SUMOylation to transcriptional control, DNA repair pathways, mitotic progression, and oncogenic signalling has been described. Here we review functions of the SUMO pathway in PDAC, with a special focus on its connection to an aggressive subtype of the disease characterised by high MYC activity, and discuss SUMOylation inhibitors under development for precise PDAC therapies.

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Section: Inhibitors Of the Sumo Pathwaymentioning

confidence: 90%

Section: Inhibitors Of the Sumo Pathwaymentioning

confidence: 90%

Section: The Sumo Pathway In Pdacmentioning

confidence: 99%

Section: Inhibitors Of the Sumo Pathwaymentioning

confidence: 99%

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The SUMO pathway in pancreatic cancer: insights and inhibition

et al. 2020

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“…In addition, many components of the SUMO pathway, including E1, E2, and several PIAS E3 proteins were shown to be highly expressed in both B-cell lymphomas and pancreatic cancer overexpressing c-Myc. This results in higher overall SUMO conjugation and consequent vulnerability of these tumors to inhibition of SUMOylation (Hoellein et al, 2014;Biederstädt et al, 2020). Finally, we have recently shown that the SUMO pathway plays an important role, on one side, in the response of acute myeloid leukemias (AML) to standard chemotherapies (Bossis et al, 2014) and, on the other side, in the resistance of nonpromyelocytic AML to differentiation therapies using retinoic acid (Baik et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

Ubiquitin and SUMO conjugation as biomarkers of acute myeloid leukemias response to chemotherapies

et al. 2020

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Ubiquitin and the ubiquitin-like SUMO are covalently conjugated to thousands of proteins to modulate their function and fate. Many of the enzymes involved in their conjugation are dysregulated in cancers and involved in cancer cell response to therapies. We describe here the identification of biomarkers of the activity of these enzymes and their use to predict acute myeloid leukemias (AML) response to standard chemotherapy (daunorubicin-DNR and cytarabine-Ara-C). We compared the ability of extracts from chemosensitive and chemoresistant AML cells to conjugate ubiquitin or SUMO-1 on 9,000 proteins spotted on protein arrays. We identified 122 proteins whose conjugation by these posttranslational modifiers marks AML resistance to DNR and/or Ara-C. Based on this signature, we defined a statistical score predicting AML patient response to standard chemotherapy. We finally developed a miniaturized assay allowing for easy assessment of modification levels of the selected biomarkers and validated it in patient cell extracts. Thus, our work identifies a new type of ubiquitin-based biomarkers that could be used to predict cancer patient response to treatments.

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Targeting the ubiquitin‐proteasome system in a pancreatic cancer subtype with hyperactive MYC

et al. 2020

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The myelocytomatosis oncogene (MYC) is an important driver in a subtype of pancreatic ductal adenocarcinoma (PDAC). However, MYC remains a challenging therapeutic target, therefore identifying druggable synthetic lethal interactions in MYC-active PDAC may lead to novel precise therapies. First, to identify networks with hyperactive MYC, we profiled transcriptomes of established human cell lines, murine primary PDAC cell lines and accessed publicly available repositories to analyze transcriptomes of primary human PDAC. Networks active in MYC hyperactive subtypes were analyzed by gene set enrichment analysis. Next, we performed an unbiased pharmacological screen to define MYC-associated vulnerabilities. Hits were validated by analysis of drug-response repositories and genetic gain-and loss-of-function experiments. In these experiments, we discovered that the proteasome inhibitor Bortezomib triggers a MYC-associated vulnerability. In addition, by integrating publicly available data, we found the unfolded protein response as a signature connected to MYC. Furthermore, increased sensitivity of MYC-hyperactive PDACs to Bortezomib was validated in genetically modified PDAC cells. In sum, we provide evidence that perturbing the ubiquitin proteasome system might be an option to target MYC hyperactive PDAC cells. Our data provide the rationale to further develop precise targeting of the ubiquitin-proteasome system as a subtype-specific therapeutic approach.

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SUMO pathway inhibition targets an aggressive pancreatic cancer subtype

Cited by 72 publications

References 59 publications

The SUMO pathway in pancreatic cancer: insights and inhibition

The SUMO pathway in pancreatic cancer: insights and inhibition

Ubiquitin and SUMO conjugation as biomarkers of acute myeloid leukemias response to chemotherapies

Targeting the ubiquitin‐proteasome system in a pancreatic cancer subtype with hyperactive MYC

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