Martina Brucoli scite author profile

Exploiting oxidative stress has recently emerged as a plausible strategy for treatment of human cancer, and antioxidant defenses are implicated in resistance to chemotherapy and radiotherapy. Targeted suppression of antioxidant defenses could thus broadly improve therapeutic outcomes. Here, we identify the AMPK-related kinase NUAK1 as a key component of the antioxidant stress response pathway and reveal a specific requirement for this role of NUAK1 in colorectal cancer. We show that NUAK1 is activated by oxidative stress and that this activation is required to facilitate nuclear import of the antioxidant master regulator NRF2: Activation of NUAK1 coordinates PP1β inhibition with AKT activation in order to suppress GSK3β-dependent inhibition of NRF2 nuclear import. Deletion of NUAK1 suppresses formation of colorectal tumors, whereas acute depletion of NUAK1 induces regression of preexisting autochthonous tumors. Importantly, elevated expression of NUAK1 in human colorectal cancer is associated with more aggressive disease and reduced overall survival. This work identifies NUAK1 as a key facilitator of the adaptive antioxidant response that is associated with aggressive disease and worse outcome in human colorectal cancer. Our data suggest that transient NUAK1 inhibition may provide a safe and effective means for treatment of human colorectal cancer via disruption of intrinsic antioxidant defenses. .

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Autophagy suppresses the formation of hepatocyte-derived cancer-initiating ductular progenitor cells in the liver

Barthet

Brucoli

Ladds

et al. 2021

Sci. Adv.

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Hepatocellular carcinoma (HCC) is driven by repeated rounds of inflammation, leading to fibrosis, cirrhosis, and, ultimately, cancer. A critical step in HCC formation is the transition from fibrosis to cirrhosis, which is associated with a change in the liver parenchyma called ductular reaction. Here, we report a genetically engineered mouse model of HCC driven by loss of macroautophagy and hemizygosity of phosphatase and tensin homolog, which develops HCC involving ductular reaction. We show through lineage tracing that, following loss of autophagy, mature hepatocytes dedifferentiate into biliary-like liver progenitor cells (ductular reaction), giving rise to HCC. Furthermore, this change is associated with deregulation of yes-associated protein and transcriptional coactivator with PDZ-binding motif transcription factors, and the combined, but not individual, deletion of these factors completely reverses the dedifferentiation capacity and tumorigenesis. These findings therefore increase our understanding of the cell of origin of HCC development and highlight new potential points for therapeutic intervention.

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XIAP as a Target of New Small Organic Natural Molecules Inducing Human Cancer Cell Death

Muñoz

Brucoli

Zecchini

et al. 2019

Cancers

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X-linked inhibitor of apoptosis protein (XIAP) is an emerging crucial therapeutic target in cancer. We report on the discovery and characterisation of small organic molecules from Piper genus plants exhibiting XIAP antagonism, namely erioquinol, a quinol substituted in the 4-position with an alkenyl group and the alkenylphenols eriopodols A–C. Another isolated compound was originally identified as gibbilimbol B. Erioquinol was the most potent inhibitor of human cancer cell viability when compared with gibbilimbol B and eriopodol A was listed as intermediate. Gibbilimbol B and eriopodol A induced apoptosis through mitochondrial permeabilisation and caspase activation while erioquinol acted on cell fate via caspase-independent/non-apoptotic mechanisms, likely involving mitochondrial dysfunctions and aberrant generation of reactive oxygen species. In silico modelling and molecular approaches suggested that all molecules inhibit XIAP by binding to XIAP-baculoviral IAP repeat domain. This demonstrates a novel aspect of XIAP as a key determinant of tumour control, at the molecular crossroad of caspase-dependent/independent cell death pathway and indicates molecular aspects to develop tumour-effective XIAP antagonists.

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ATG7 is a haploinsufficient repressor of tumor progression and promoter of metastasis

Long

Kania

McEwan

et al. 2022

Proc. Natl. Acad. Sci. U.S.A.

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The role of autophagy in cancer is complex. Both tumor-promoting and tumor-suppressive effects are reported, with tumor type, stage and specific genetic lesions dictating the role. This calls for analysis in models that best recapitulate each tumor type, from initiation to metastatic disease, to specifically understand the contribution of autophagy in each context. Here, we report the effects of deleting the essential autophagy gene Atg7 in a model of pancreatic ductal adenocarcinoma (PDAC), in which mutant Kras G12D and mutant Trp53 172H are induced in adult tissue leading to metastatic PDAC. This revealed that Atg7 loss in the presence of Kras G12D /+ and Trp53 172H /+ was tumor promoting, similar to previous observations in tumors driven by embryonic Kras G12D /+ and deletion of Trp53 . However, Atg7 hemizygosity also enhanced tumor initiation and progression, even though this did not ablate autophagy. Moreover, despite this enhanced progression, fewer Atg7 hemizygous mice had metastases compared with animals wild type for this allele, indicating that ATG7 is a promoter of metastasis. We show, in addition, that Atg7 +/− tumors have comparatively lower levels of succinate, and that cells derived from Atg7 +/− tumors are also less invasive than those from Atg7 +/+ tumors. This effect on invasion can be rescued by ectopic expression of Atg7 in Atg7 +/− cells, without affecting the autophagic capacity of the cells, or by treatment with a cell-permeable analog of succinate. These findings therefore show that ATG7 has roles in invasion and metastasis that are not related to the role of the protein in the regulation of autophagy.

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Figures S1-S6 & Tables S1 & S2 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Port¹,

Muthalagu²,

Raja³

et al. 2023

Preprint

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Figures S1-S6 & Tables S1 & S2 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Port¹,

Muthalagu²,

Raja³

et al. 2023

Preprint

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Supplementary Table 3 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Port¹,

Muthalagu²,

Raja³

et al. 2023

Preprint

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Supplementary Table 3 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Port¹,

Muthalagu²,

Raja³

et al. 2023

Preprint

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Martina Brucoli

Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Autophagy suppresses the formation of hepatocyte-derived cancer-initiating ductular progenitor cells in the liver

XIAP as a Target of New Small Organic Natural Molecules Inducing Human Cancer Cell Death

ATG7 is a haploinsufficient repressor of tumor progression and promoter of metastasis

Figures S1-S6 & Tables S1 & S2 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Figures S1-S6 & Tables S1 & S2 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Supplementary Table 3 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

Supplementary Table 3 from Colorectal Tumors Require NUAK1 for Protection from Oxidative Stress

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