The merits of vascular targeting for gynecologic malignancies

Kamat, Aparna A.; Sood, Anil K.

doi:10.1007/s11912-005-0009-x

Cited by 2 publications

(1 citation statement)

References 57 publications

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“…Bevacizumab was the first anti-vascular agent to receive approval from the Food & Drug Administration (FDA) for clinical use when given in combination with chemotherapy based on results from a phase III trial showing a 4.7 month improvement in overall survival in previously untreated, metastatic colorectal cancer patients [52]. We have previously reported the benefits of developing agents that target specific components of the vascular system and their potential role in ovarian cancer therapy [58]. Furthermore, we have shown in pre-clinical models that targeting genes responsible for angiogenesis with novel therapeutic strategies, such as siRNA targeted therapy, has therapeutic efficacy and these approaches are being developed clinically [65,66].…”

Section: Activatorsmentioning

confidence: 99%

Markers of Angiogenesis in Ovarian Cancer

Merritt

Sood

2007

Disease Markers

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Tumor development and progression are inherently dependent on the process of angiogenesis. Recently, anti-angiogenic therapy has started to show promise as an effective treatment strategy in many solid tumors including ovarian carcinoma. Unfortunately, lack of effective biomarkers presents a challenge for oncologists in treatment planning as well as monitoring response of new anti-vascular agents. Previously, quantification of angiogenesis by microvessel density analysis provided useful prognostic information, however, its utility following anti-angiogenic therapy remains to be determined. Moreover, since secreted cytokines play an active part in angiogenesis by mediating neovascularization in tumors, investigations have focused on their potential role to serve as candidate biomarkers of disease detection, prognosis, and treatment response. In this article, we review the role of key angiogenesis markers as potential biomarkers in ovarian carcinoma.

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Section: Activatorsmentioning

confidence: 99%

Markers of Angiogenesis in Ovarian Cancer

Merritt

Sood

2007

Disease Markers

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Molecular Technologies in Gynecologic Oncology

Comparetto

Borruto

2015

J. Can. Res. Updates

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In recent years, the application of molecular biological techniques to the diagnosis and treatment of cancer has proved successful. In this kind of pathologies, molecular diagnosis is of fundamental importance as it allows identification at a pre-symptomatic stage, and then in the early phase, of the subjects in which cancer disease is developing. Molecular diagnosis of tumors by deoxy-ribonucleic acid (DNA) analysis is conducted on biological samples such as urine, feces, sputum, vaginal swab, and blood, searching and identifying in the various samples for the presence of cell carriers of an altered genetic information. The sensitivity of this kind of analysis is so high as to be very reliable even in the presence in the sample of a few tumor cells, level not reachable through the traditional “tumor markers”. The achievement of a facilitated early diagnosis of the tumor and, consequently, through the organization of specific therapeutic interventions, the prevention of the invasiveness of the pathology, allow to insert this kind of analysis among the most important investigations in the field of cancer prevention. Molecular oncology examinations have targeted the mutational study of the most involved genes in the onset of hereditary and/or family cancers such as breast, ovary, colon, melanoma, stomach, thyroid, etc. In addition, given the growing focus on the molecular mechanisms underlying the individual response to conventional chemotherapeutic drugs and molecular targeted agents responsible for drug resistance, pharmacogenetics exams have been added to those of molecular oncology. Some genes, when altered and/or mutated, can cause the development of tumors. In some types of cancer, the mutation may affect only somatic cells: in this case, the development will manifest itself only in the subject carrier of the mutation. Otherwise, if the mutation affects germ cells genes, it may occur the possibility to convey to children a susceptibility to the development of tumors. In fact, a significant proportion of cancers are hereditary. For example, it is estimated that about 7% of breast cancers, 10% of ovarian cancers, and about 5-10% of colorectal cancers, are caused by recurrent mutations at specific genes level. The early detection of cancer, with the ability to identify individuals at risk of developing the disease, is now the best way to reduce mortality from it. Determining whether a person has a mutation in a gene involved in neoplastic transformation that predisposes to the development of cancer (susceptibility or genetic predisposition) can significantly decrease its incidence and mortality. For example, as a result of in-depth studies of families at risk, it has been estimated that women who have inherited mutations in breast cancer genes (BRCA1 or BRCA2) are likely to develop breast cancer in 87% of cases, compared with 10% of non-bearers. This probability falls to 44-60% in the case of ovarian cancer, compared with 1% probability of not carriers. In this area, basic research has been developed with the aim of contributing to the study of the molecular mechanisms of oncogenesis, which generally has multistage character, with an initial immortalization and cell transformation and subsequent tumor progression. In this regard, studies at the molecular and functional level have been focused on models of different types of cancer, e.g. melanoma. In parallel, it has been studied the possible oncogenetic role of certain families of genes that have a functional role in embryogenesis, and in general in cell proliferation/differentiation, e.g. homeotic (HOX) genes. The gene expression profiles of purified cancer cells can be evaluated by microarray technique, comparing them with those of normal cells: comparative analysis, based on specific software, allows the identification of genes selectively modulated in the genetic program of tumor cells, in particular of genes specifically involved in the onset and progression of tumors. The modern goal of cancer therapy is to eliminate the disease by minimizing trauma and paying attention to the quality of life (QOL). With the passing of time, there has been a change of therapeutic paradigms and we have gone from the objective of maximum tolerable treatment to that of minimum effective treatment. This clinical imperative has its foundation in the quick transfer of biological knowledges to the care, integrating molecular informations with the development of new treatment methods. Especially for a delicate operation, even psychologically, such as that for breast cancer. In this setting, we have focused particularly on the technique of sentinel lymph node, demonstrating the possibility to avoid the treatment of the axilla in patients at low risk of recurrence. The term “molecular targeted therapy” is used to refer to agents that target specific pathways activated in the processes of growth, survival, invasion, and metastasis of cancer cells and in tumor neo-angiogenesis. The large and perhaps excessive optimism, caused by the gradual deepening of the knowledges of these mechanisms, has received a further boost by the arrival on the therapeutic scene of imatinib and other drugs belonging to the class of targeted biomolecular agents, including some monoclonal antibodies (McAb) such as trastuzumab, rituximab, cetuximab, and bevacizumab, and some small molecules, already entered clinical practice. But the question we must ask is whether that enthusiasm is justified and supported by scientifically strong and clinically proven data. The difficulties encountered in the research and development of new truly effective molecules and the disappointing results obtained in the early life of some of these agents and, not least, the high costs of treatments must lead to greater caution. The medical oncologist has the inescapable duty to possess sufficient culture to be able to properly use these new therapies in his diagnosis and treatment decision-making.

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The merits of vascular targeting for gynecologic malignancies

Cited by 2 publications

References 57 publications

Markers of Angiogenesis in Ovarian Cancer

Markers of Angiogenesis in Ovarian Cancer

Molecular Technologies in Gynecologic Oncology

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