Tumor suppressor genes in differentiation and oncogenesis (Prof. Collavin)

Research Strand:

Full professor in Applied Biology (BIO/13)

Tel: +39-040-5588741
email: lcollavin@units.it

Biosketch

Graduated in Biological Sciences, Licio Collavin obtained his PhD from the International School for Advanced Studies (SISSA) in Trieste, working in the group of prof. Claudio Schneider, at LNCIB. Next, he did a three years postdoc in the lab of prof. Marc W. Kirschner, in the Department of Cell Biology at Harvard Medical School, Boston MA (USA). In 2003, dr. Collavin became Assistant Professor (Ricercatore) at the University of Trieste, and moved back to LNCIB as principal investigator (PI). Since 2020, the Collavin lab has moved to the main campus of the University.

His most significant scientific contributions include:
- The identification of novel genes regulated by the tumor suppressor p53 and the discovery of a membrane isoform of the enzyme Adenylate Kinase 1 (Utrera et al., 1998; Collavin et al., 1999).
- The discovery of a negative feedback loop, mediated by the extracellular protein Sizzled, which regulates ventral mesoderm differentiation during and after gastrulation in the amphibian Xenopus laevis (Collavin and Kirschner, 2003).
- The identification of novel interactors of the p53 protein family, evolutionarily conserved from Drosophila to humans (Lunardi et al., 2010).
- The characterization of the tumor suppressor DAB2IP as a critical functional target of mutant p53, mediating pro-oncogenic responses in cancer cells exposed to inflammation (Di Minin et al., 2014) or insulin (Valentino et al., 2017).
- The discovery that mutant forms of p53 can modulate the endoplasmic reticulum stress response in cancer cells (Sicari et al., 2019).
- The observation that the tumor suppressor DAB2IP contributes to the negative regulation of the oncogenic factors YAP/TAZ in epithelial cells under conditions of high cell density or confluence (Apollonio et al., 2023).

Info

Research

Research

We are interested in the molecular basis of cancer. We aim to help understand the molecular mechanisms that drive cancer progression and aggressiveness, as well as the mechanisms that regulate the complex interaction of cancer cells with their environment, including other cells and the immune system. Our approach is to look at functional interactions between tumor suppressor genes and signaling pathways that control physiological and pathological cell activities.

1) Exploring the gain-of-function properties of mutant p53 through novel interacting proteins

In human cancers, tumor suppressor gene TP53 is mutated very frequently. Notably, about 70% of TP53 mutations are missense, inducing single aminoacid substitutions in the p53 protein. Therefore, many tumors express mutant p53 proteins that not only lose their normal tumor-suppressive functions, but also acquire novel oncogenic properties (a phenomenon called gain-of-function), as they in fact promote cancer progression and drug resistance. Accordingly, tumors with mutant p53 tend to be more aggressive, and are often associated with worst prognosis.

The mechanism underlying the gain of function partly depends on the interaction with other cellular proteins. In fact, tumor-associated p53 mutations may drastically alter the protein interaction profile of p53. For instance, they may prevent interaction with certain proteins, while binding to other proteins may remain unaffected. Alternatively, mutant p53 (mutp53) could acquire the capability to interact with cellular proteins that normally do not bind wild-type p53. For this reason, there is considerable interest in defining the interaction profile of oncogenic p53 mutants as compared to that of wild-type p53.

Various years ago, we searched the Drosophila genome for proteins that interact in vitro with the single p53 protein (Dmp53) in this organism. We reasoned that an unbiased "phylogenetic" approach could reveal novel, highly conserved molecular circuits regulating this very important tumor suppressor pathway in mammals. We used the Drosophila hits as a framework to study the corresponding interactions in mammals. We tested the human orthologs of 41 newly discovered Dmp53 interactors for association with human p53, p73 and p63, and obtained a list of 37 potential partners of these crucial tumor suppressor proteins (Lunardi et al., 2010).

As a follow-up of this work, we systematically tested the novel interactors for their binding to mutant p53(H175R). Notably, a consistent fraction of the proteins bound to mutant p53 (unpublished data). Thus, we are studying the possible role of these mutp53 interactors in the gain of function phenotype associated to oncogenic p53 mutants.

Recently, we discovered that expression of mutant p53 enhances the resistance to ER stress in cancer cell by modulating Unfolded Protein Response (UPR). We found that mutp53 inhibits activation of pro-apoptotic branches of the UPR, while it enhances activation of the pro-survival UPR effector ATF6. Data suggest that pharmacological inhibition of mutp53 could be combined with ATF6 inhibitors to sensitize cancer cells to chemotherapy (Sicari et al., 2019).

2) The tumor suppressor DAB2IP as a target for post transcriptional inactivation in cancer

The dynamic crosstalk between tumor cells and tumor stroma is a major determinant of cancer aggressiveness. In this context, signaling modulators that control specificity, amplitude, and duration of cell responses to extrinsic inputs can play a crucial role - often underestimated.

The tumor suppressor DAB2IP/AIP1 belongs to this category; is a cytoplasmic Ras inhibitor (Ras-GAP) that also restrains NF-kB activation by inflammatory cytokines, and PI3K-AKT activation by various growth factors. There are solid evidences that DAB2IP loss-of-function in cancer cells enhances their aggressiveness; accordingly, various mechanisms for DAB2IP inactivation have been described in human cancers (Bellazzo et al., 2016).

3) DAB2IP inactivation by mutant p53

We discovered that mutp53 can bind and inhibit the tumor suppressor DAB2IP, thus potentially affecting the cell’s response to a variety of extracellular inputs. Interestingly, it appears that various different tumor-associated p53 mutants can bind DAB2IP, regardless of the specific missense mutation; this suggests that this interaction may be a general feature of mutp53 proteins, so this molecular axis may be an attractive target for therapeutic strategies.

Functionally speaking, we found that mutant p53, by binding DAB2IP in the cytoplasm, alters the response of cancer cells to TNF, increasing their aggressiveness in response to inflammation (Di Minin et al., 2014). We also found that the mutp53-DAB2IP interaction affects the response of cancer cells to Insulin, causing enhanced and prolonged AKT activation. This finding revealed a potential impact of p53 mutation in breast tumors that develop in hyperinsulinemic obese or diabetic patients (Valentino et al., 2017).

4) DAB2IP inactivation by micro-RNA

We have identified a panel of microRNAs able to target the mRNA of DAB2IP. Among them, we characterized miRNA-149-3p as a potent antagonist of DAB2IP translation and functions. miR-149-3p expression in prostate cancer cell lines counteracts DAB2IP action, favoring an immunogenic and pro-angiogenic NF-kB-related gene expression program, and an invasive phenotype. In vivo xenograft experiments supported the in vitroresults: inhibition of miR-149-3p counteracted prostate cancer cell dissemination in nude mice, and reduced cancer cell growth and angiogenic remodeling in zebrafish larvae (Bellazzo et al., 2018).

In addition to inducing cell-autonomous effects, expression of miR-149-3p in cancer cells can possibly act also on the tumor microenvironment. We found that secreted miR-149-3p induces DAB2IP downregulation in non-transformed cell lines and in primary endothelial cells. This is a possible mechanism by which cancer cells could inactivate DAB2IP in stromal cells, to establish a supporting microenvironment that would facilitate tumor growth and dissemination. We found that miR-149-3p partially mediates this phenotype in prostate cancer cell lines, but additional factors are likely to be involved, including other DAB2IP-targeting miRNAs.

We are currently interested in understanding the mechanisms and potential impact of cell non-autonomous DAB2IP inhibition in endothelial cells, and possibly in other stromal cells. This may provide further insight on the reciprocal regulation between cancer and stroma, and may reveal novel targets for therapy.

People

Current group members

Olga Pastorino

+39 040 5588742
Olga.pastorino@units.it

Graduated in Molecular Biology at the Second University of Naples (now University of Campania L. Vanvitelli), she obtained a PhD in Biomolecular Sciences at the same University, focusing her research activity mainly on the pathological processes underlying brain tumors. Currently a postdoctoral research fellow, she is working on the project “Dissecting the impact of mutant p53 in life-death decisions of cancer cells exposed to microenvironmental stress”. In particular, the research activity carried out aims to identify the differential response of cells with different p53 status to endoplasmic reticulum stress.

Nicoletta Franco

+39 040 5588742
NICOLETTA.FRANCO@phd.units.it

Nicoletta holds a degree in Medical Biotechnology from the University of Trieste and is currently a Ph.D. student in Molecular Biomedicine at the University of Trieste. Her research focuses on investigating the mechanisms regulating DAB2IP levels in response to cell density in epithelial cells, as well as the role of DAB2IP in modulating the activity of the YAP and TAZ transcriptional regulators under conditions of cell confluence.

Arooj Fatima

+39 040 5588742
AROOJ.FATIMA@phd.units.it

Graduated in Molecular Biology at the Punjab University in Lahore, Pakistan, Arooj is currently pursuing a PhD in Molecular Biomedicine at the University of Trieste. Her research focuses on understanding the mechanisms and biological impact of cell non-autonomous DAB2IP downregulation in the reciprocal interaction between cancer cells and stromal cells.

Monica Rossin

+39 040 5588742
MONICA.ROSSIN@studenti.units.it

Graduated in Functional Genomics from the University of Trieste, Monica investigates the biological effects and mechanism of action of specific drugs that regulate DAB2IP protein levels in cancer cells, aiming to limit metastasis and enhance chemotherapy response.

Some past group members

Fulvio Chiacchiera, former PhD student (now associate professor at CIBIO, University of Trento).
Marco Dal Ferro, former PhD student and Postdoc (now at Bio4Dreams, Treiste).
Giulio Di Minin, former PhD student and Postdoc (now Postdoc at ETH, Zurich, CH).
Andrea Lunardi, former PostDoc (now associate professor at CIBIO, University of Trento).
Daria Sicari, former PhD student (now Medical Affair Specialist at Pharmaline, Milano).
Mattia Apollonio, former PhD student (now Medical Science Liaison at MSD, Roma).
Rossella De Florian Fania, former PhD student (now PostDoc at Johns' Hopkins Univeristy, USA).

Bellazzo Arianna (Research Group - Member)

Prof. Collavin Licio (Research Group - Member)
lcollavin@units.it

Sicari Daria (Research Group - Member)

Valentino Elena (Research Group - Member)

Publications

Full list of the publications of the Principal Investigator

Google scholar
Scopus

Highly cited DSV papers

2019
2014
2012
2010

Selected papers

De Florian Fania, R., Bellazzo, A., and Collavin, L. (2024). An update on the tumor-suppressive functions of the RasGAP protein DAB2IP with focus on therapeutic implications. Cell Death Differ 31, 844-854. epub: 20240620. doi: 10.1038/s41418-024-01332-3
Apollonio, M., Bellazzo, A., Franco, N., Lombardi, S., Senigagliesi, B., Casalis, L., Parisse, P., Thalhammer, A., Baj, G., De Florian Fania, R., Del Sal, G., and Collavin, L. (2023). The Tumor Suppressor DAB2IP Is Regulated by Cell Contact and Contributes to YAP/TAZ Inhibition in Confluent Cells. Cancers (Basel) 15. epub: 2023/07/14. doi: 10.3390/cancers15133379
Sicari, D., Fantuz, M., Bellazzo, A., Valentino, E., Apollonio, M., Pontisso, I., Di Cristino, F., Dal Ferro, M., Bicciato, S., Del Sal, G., and Collavin, L. (2019). Mutant p53 improves cancer cells' resistance to endoplasmic reticulum stress by sustaining activation of the UPR regulator ATF6. Oncogene 38, 6184-6195. epub: 2019/07/18. doi: 10.1038/s41388-019-0878-3
Bellazzo, A., Di Minin, G., Valentino, E., Sicari, D., Torre, D., Marchionni, L., Serpi, F., Stadler, M.B., Taverna, D., Zuccolotto, G., Montagner, I.M., Rosato, A., Tonon, F., Zennaro, C., Agostinis, C., Bulla, R., Mano, M., Del Sal, G., and Collavin, L. (2018). Cell-autonomous and cell non-autonomous downregulation of tumor suppressor DAB2IP by microRNA-149-3p promotes aggressiveness of cancer cells. Cell death and differentiation 25, 1224-1238. epub: 2018/03/22. doi: 10.1038
Valentino, E., Bellazzo, A., Di Minin, G., Sicari, D., Apollonio, M., Scognamiglio, G., Di Bonito, M., Botti, G., Del Sal, G., and Collavin, L. (2017). Mutant p53 potentiates the oncogenic effects of insulin by inhibiting the tumor suppressor DAB2IP. Proc Natl Acad Sci U S A 114, 7623-7628. doi: 10.1073/pnas.1700996114
Bellazzo, A., Di Minin, G., and Collavin, L. (2017). Block one, unleash a hundred. Mechanisms of DAB2IP inactivation in cancer. Cell Death Differ 24, 15-25. epub: 2016/11/18. doi: 10.1038/cdd.2016.134
Di Minin, G., Bellazzo, A., Dal Ferro, M., Chiaruttini, G., Nuzzo, S., Bicciato, S., Piazza, S., Rami, D., Bulla, R., Sommaggio, R., Rosato, A., Del Sal, G., and Collavin, L. (2014). Mutant p53 reprograms TNF signaling in cancer cells through interaction with the tumor suppressor DAB2IP. Molecular cell 56, 617-629. doi: 10.1016/j.molcel.2014.10.013
Collavin, L., Lunardi, A., and Del Sal, G. (2010). p53-family proteins and their regulators: hubs and spokes in tumor suppression. Cell Death Differ 17, 901-911. epub: 2010/04/10. doi: 10.1038/cdd.2010.35
Lunardi, A., Di Minin, G., Provero, P., Dal Ferro, M., Carotti, M., Del Sal, G., and Collavin, L. (2010). A genome-scale protein interaction profile of Drosophila p53 uncovers additional nodes of the human p53 network. Proc Natl Acad Sci U S A 107, 6322-6327. epub: 2010/03/24. doi: 10.1073/pnas.1002447107
Mauri, F., McNamee, L.M., Lunardi, A., Chiacchiera, F., Del Sal, G., Brodsky, M.H., and Collavin, L. (2008). Modification of Drosophila p53 by SUMO modulates its transactivation and pro-apoptotic functions. J Biol Chem 283, 20848-20856. epub: 2008/05/22. doi: 10.1074/jbc.M710186200

Notices

If you are interested in joining the Collavin group,
please send a self-presentation letter and CV to the following address:

lcollavin@units.it

Last update: 02-27-2025 - 13:22

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