11 results on '"Target therapies"'
Search Results
2. Advances in understanding the mechanisms of evasive and innate resistance to mTOR inhibition in cancer cells.
- Author
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Chiarini, Francesca, Evangelisti, Camilla, Lattanzi, Giovanna, McCubrey, James A., and Martelli, Alberto M.
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NATURAL immunity , *CANCER cells , *MTOR inhibitors , *DISEASE progression - Abstract
The development of drug-resistance by neoplastic cells is recognized as a major cause of targeted therapy failure and disease progression. The mechanistic (previously mammalian) target of rapamycin (mTOR) is a highly conserved Ser/Thr kinase that acts as the catalytic subunit of two structurally and functionally distinct large multiprotein complexes, referred to as mTOR complex 1 (mTORC1) and mTORC2. Both mTORC1 and mTORC2 play key roles in a variety of healthy cell types/tissues by regulating physiological anabolic and catabolic processes in response to external cues. However, a body of evidence identified aberrant activation of mTOR signaling as a common event in many human tumors. Therefore, mTOR is an attractive target for therapeutic targeting in cancer and this fact has driven the development of numerous mTOR inhibitors, several of which have progressed to clinical trials. Nevertheless, mTOR inhibitors have met with a very limited success as anticancer therapeutics. Among other reasons, this failure was initially ascribed to the activation of several compensatory signaling pathways that dampen the efficacy of mTOR inhibitors. The discovery of these regulatory feedback mechanisms greatly contributed to a better understanding of cancer cell resistance to mTOR targeting agents. However, over the last few years, other mechanisms of resistance have emerged, including epigenetic alterations, compensatory metabolism rewiring and the occurrence of mTOR mutations. In this article, we provide the reader with an updated overview of the mechanisms that could explain resistance of cancer cells to the various classes of mTOR inhibitors. • Aberrant activation of mTOR is a common event in human tumors, making mTOR an attractive target for cancer therapy. • mTOR inhibitors have met with a very limited success as anticancer therapeutics. • Understanding the reasons underlying the lack of efficacy of mTOR inhibition is important for the design of better therapies. • mTOR inhibitors unleash activation of several compensatory signaling pathways that dampen their efficacy. • However other mechanisms of resistance emerged, including epigenetic changes, compensatory metabolism and mTOR mutations. [ABSTRACT FROM AUTHOR]
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- 2019
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- View/download PDF
3. New molecular therapies in patients with advanced Hepatocellular Cancer in second line of treatment: Is a real defeat?: Results from a literature based meta-analysis of randomized trials.
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Roviello, Giandomenico, Zanotti, Laura, Cappelletti, Maria Rosa, Gobbi, Angela, Borsella, Giulia, Pacifico, Chiara, Multari, Andrea Giovanni, and Generali, Daniele
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LIVER cancer , *LIVER cancer patients , *TARGETED drug delivery , *TREATMENT effectiveness , *RANDOMIZED controlled trials - Abstract
Several new biological agents have been investigated as second line of treatment in advanced Hepatocellular Cancer (HCC). We performed a meta -analysis to assess the effect of targeted therapies in advanced HCC patients beyond the first line of treatment. A literature-based metaanalysis of randomized controlled trials was undertaken. The primary outcome was the overall survival. The secondary endpoints were the progression-free survival (PFS), the response rate (RR) and disease control rate (DCR) and the safety. Pooled analysis of targeted agents revealed a modest increase in overall survival compared with control arm (Hazard Ratio (HR) = 0.93, 95%CI: 0.83-1.04; P = 0.21). On the counterpart, all the secondary endpoints were in favoured to the targeted agents-based treatment (PFS: HR = 0.68, 95% CI:0.56–0.83; P = 0.0002; RR: 3.50,95% CI 1.81–6.76; P = 0.0002, DCR: RR:1.19, 95% CI 1.06–1.32; P = 0.002). To date, there is a clinical need of a more efficacious second line of therapy in treatment of the advanced HCC. This study showed some activity of the new targeted therapies in second line of treatment in advanced HCC. [ABSTRACT FROM AUTHOR]
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- 2016
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4. Emerging toxicities in the treatment of non-small cell lung cancer: Ocular disorders.
- Author
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Agustoni, Francesco, Platania, Marco, Vitali, Milena, Zilembo, Nicoletta, Haspinger, Eva, Sinno, Valentina, Gallucci, Rosaria, de Braud, Filippo, and Garassino, Marina Chiara
- Abstract
Abstract: The treatment of advanced disease (stage IIIb and IV) of non-small cell lung cancer (NSCLC) is based on systemic treatment with platinum-based chemotherapy or biological compounds depending on the disease molecular profile. In the last few years, intensive investigational efforts in anticancer therapy have led to the registration of new active chemotherapeutic agents, combination regimens, and biological drugs, expanding choices for customizing individual treatment. However, the introduction of new drugs in the clinical setting has led to several new toxicities, creating some difficulties in daily management. Among these, ocular toxicity is generally overlooked as more common toxicities such as myelosuppression, stomatitis, diarrhea, vomiting, “hand–foot syndrome”, and neurological alterations attract greater attention. Ophthalmic complications from cytotoxic chemotherapeutics are rare, transient, and of mild/moderate intensity but irreversible acute disorders are possible. The best way to prevent potential irreversible visual complications is an awareness of the potential for ocular toxicity because dose reductions or early drug cessation can prevent serious ocular complications in the majority of cases. However, given the novelty of many therapeutic agents and the complexity of ocular pathology, oncologists may be unfamiliar with these adverse effects of anticancer therapy. Although toxicities from chemotherapy are generally intense but short lasting, toxicities related to targeted drugs are often milder but longer lasting and can persist throughout treatment. Here we review the principal clinical presentations of ocular toxicity arising from chemotherapy [1–3], target therapies [4], and newly developed drugs and provide some recommendations for monitoring and management of ocular toxicity. [Copyright &y& Elsevier]
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- 2014
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5. Italian practical clinical guidelines on cholangiocarcinoma: Part II, treatment
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Alvaro, D., Hassan, C., Cardinale, V., Carpino, G., Fabris, L., Gringeri, E., Granata, V., Mutignani, M., Morement, H., Giuliante, F., Guglielmi, A., Ridola, L., Tonini, G., Marzioni, M., Grazi, G., Guido, M., Di Giulio, E., Pantano, F., Venere, R., Bragazzi, M. C., Biancanello, F., Faccioli, J., Giannetti, A., Cintolo, M., Di Giunta, M., Gambato, M., Lasagni, A., Izzo, F., Avallone, A., Banales, J., Rossi, M., Catalano, C., Laghi, A., D'Amati, G., and Mancino, M. G.
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surgery ,distal cholangiocarcinoma ,intrahepatic cholangiocarcinoma ,liver transplantation ,locoregional treatments ,perihilar cholangiocarcinoma ,target therapies - Published
- 2020
6. Thymoma and thymic carcinoma in the target therapies era.
- Author
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Lamarca, Angela, Moreno, Victor, and Feliu, Jaime
- Abstract
Summary: Thymic malignancies are extremely rare although usually affect young adults and continue to remain an important health problem. Like other rare diseases, progress in thymic malignancies has been slow and the treatment cornerstone still remains surgical resection. Next generation sequencing and other advances in molecular biology are shedding light onto the multiple genetic aberrations involved and have opened a new field for research with molecularly targeted therapies such as CKIT inhibitors or anti-EGFR therapies. In this review we will summarize the current knowledge in the pathophysiology, diagnosis, prognosis and latest advances in the management of thymomas and thymic carcinomas. [Copyright &y& Elsevier]
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- 2013
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7. Women and lung cancer: Clinical and molecular profiling as a determinate for treatment decisions: A literature review
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Berardi, Rossana, Verdecchia, Lorena, Paolo, Marzia Di Pietro, Giampieri, Riccardo, Scartozzi, Mario, Pierantoni, Chiara, Bianconi, Maristella, Mazzanti, Paola, and Cascinu, Stefano
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LUNG cancer treatment , *CANCER in women , *MOLECULAR biology , *THERAPEUTICS - Abstract
Abstract: In the past decade the incidence of lung cancer among women has risen, whereas among men it has slightly declined. Important differences in lung cancer have been demonstrated between men and women, although many areas still remain controversial. Some biologic differences may justify the increase in response of women to therapy for lung cancer and can partially explain the improved survival of women compared with men. We extensively reviewed the published scientific literature on this topic in order to investigate the clinical and genetic profiling underlying lung cancer in women and to use this information as a tool for medical therapy. [Copyright &y& Elsevier]
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- 2009
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8. Biliary tract cancers: Molecular profiling as a tool for treatment decisions. A literature review.
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Rossana, Berardi, Mario, Scartozzi, Federica, Freddari, Michela, Squadroni, Alfredo, Santinelli, Italo, Bearzi, Guidalberto, Fabris, and Stefano, Cascinu
- Abstract
Summary: Biliary tract cancer is a quite rare disease; despite recent significant advances in imaging modalities, most of the patients have advanced disease at presentation thus making radical surgery not feasible. Many different chemotherapeutic regimens have been investigated in small uncontrolled studies, with generally disappointing results. We extensively reviewed the literature on this topic trying to give an explanation to chemoresistance in this setting of patients and considering the molecular profiling as a tool for treatment decision. This review is divided in two parts, in the first one we illustrated chemotherapy results and possible mechanisms of resistance. In the second part we analysed the new molecular targets developing an hypothesis about the future therapeutics perspectives. [Copyright &y& Elsevier]
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- 2006
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9. Crosstalks of GSK3 signaling with the mTOR network and effects on targeted therapy of cancer.
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Evangelisti, Camilla, Chiarini, Francesca, Paganelli, Francesca, Marmiroli, Sandra, and Martelli, Alberto M.
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CANCER treatment , *NETWORK effect , *MTOR inhibitors , *GLYCOGEN synthase kinase-3 , *NATURAL immunity - Abstract
The introduction of therapeutics targeting specific tumor-promoting oncogenic or non-oncogenic signaling pathways has revolutionized cancer treatment. Mechanistic (previously mammalian) target of rapamycin (mTOR), a highly conserved Ser/Thr kinase, is a central hub of the phosphatidylinositol 3-kinase (PI3K)/Akt/mTOR network, one of the most frequently deregulated signaling pathways in cancer, that makes it an attractive target for therapy. Numerous mTOR inhibitors have progressed to clinical trials and two of them have been officially approved as anticancer therapeutics. However, mTOR-targeting drugs have met with a very limited success in cancer patients. Frequently, the primary impediment to a successful targeted therapy in cancer is drug-resistance, either from the very beginning of the therapy (innate resistance) or after an initial response and upon repeated drug treatment (evasive or acquired resistance). Drug-resistance leads to treatment failure and relapse/progression of the disease. Resistance to mTOR inhibitors depends, among other reasons, on activation/deactivation of several signaling pathways, included those regulated by glycogen synthase kinase-3 (GSK3), a protein that targets a vast number of substrates in its repertoire, thereby orchestrating many processes that include cell proliferation and survival, metabolism, differentiation, and stemness. A detailed knowledge of the rewiring of signaling pathways triggered by exposure to mTOR inhibitors is critical to our understanding of the consequences such perturbations cause in tumors, including the emergence of drug-resistant cells. Here, we provide the reader with an updated overview of intricate circuitries that connect mTOR and GSK3 and we relate them to the efficacy (or lack of efficacy) of mTOR inhibitors in cancer cells. • Playing key roles in neoplastic cell pathophysiology, mTOR is an attractive target for cancer therapy. • mTOR inhibitors have met with an extremely limited success in cancer patients. • It is critical to better understand the reasons underlying the lack of efficacy of mTOR inhibition. • mTOR inhibitors cause the rewiring of several signaling pathways that dampen their efficacy. • GSK3 is emerging as a major player orchestrating resistance to mTOR-targeted therapeutics. [ABSTRACT FROM AUTHOR]
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- 2020
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10. Delving into PARP inhibition from bench to bedside and back.
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Grignani, Giovanni, Merlini, Alessandra, Sangiolo, Dario, D'Ambrosio, Lorenzo, and Pignochino, Ymera
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POLY(ADP-ribose) polymerase , *CLINICAL indications , *TUMOR microenvironment , *BENCHES , *CLINICAL pharmacology - Abstract
With the ever-expanding therapeutic indications and ongoing clinical trials with Poly(adenosine diphosphate-ribose) Polymerase (PARP) inhibitors, it is of outmost importance to stop and rethink what we know and still do not know concerning one of the major revolutions in target therapies in the last decades. Indeed, many PARP inhibitors (PARPi) are able to bind multiple targets, with a plethora of potential interactions with cancer cell signaling, metabolism and the tumor microenvironment (TME). These interactions can mediate both response and resistance to PARPi, but also represent an opportunity for sequential and/or combinatorial therapies. Here we advocate a "look before you leap" approach in reviewing available clinical and preclinical evidence concerning PARPi, delving into this complex entanglement, trying to unravel the potential for innovative therapeutic strategies revolving on PARP inhibition. [ABSTRACT FROM AUTHOR]
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- 2020
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11. New advances in targeting aberrant signaling pathways in T-cell acute lymphoblastic leukemia.
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Paganelli, Francesca, Lonetti, Annalisa, Anselmi, Laura, Martelli, Alberto M., Evangelisti, Camilla, and Chiarini, Francesca
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LYMPHOBLASTIC leukemia , *ACUTE leukemia , *PATHOLOGY , *CELL growth , *SMALL molecules - Abstract
T-cell acute lymphoblastic leukemia (T-ALL) is an aggressive disorder characterized by malignant transformation of immature progenitors primed towards T-cell development. Over the past 15 years, advances in the molecular characterization of T-ALL have uncovered oncogenic key drivers and crucial signaling pathways of this disease, opening new chances for the development of novel therapeutic strategies. Currently, T-ALL patients are still treated with aggressive therapies, consisting of high dose multiagent chemotherapy. To minimize and overcome the unfavorable effects of these regimens, it is critical to identify innovative targets and test selective inhibitors of such targets. Major efforts are being made to develop small molecules against deregulated signaling pathways, which sustain T-ALL cell growth, survival, metabolism, and drug-resistance. This review will focus on recent improvements in the understanding of the signaling pathways involved in the pathogenesis of T-ALL and on the challenging opportunities for T-ALL targeted therapies. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
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