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Featured researches published by Sabin Cinca.


Journal of Translational Medicine | 2015

Clinical value of Melanoma Inhibitory Activity in stratifying malignant melanoma patients

Angela Sandru; Silviu Voinea; Eugenia Panaitescu; Madalina Bolovan; Adina Stanciu; Sabin Cinca; Alexandru Blidaru

Background Malignant melanoma (MM) is a heterogeneous disease, well-known for its unpredictable clinical course and lack of response to most systemic therapies. Furthermore in some parts of the world it has quite an epidemic nature, with an incidence that has increased steadily in the last 30 years [1]. Therefore the characterization of new tumor markers that could better suggest the patient outcome has become a priority for many research centers. Melanoma Inhibitory Activity (MIA) is a protein highly expressed and secreted by malignant melanocytes [1,2], without being identified in benign melanocytes or other normal skin cells [3]. More, the induction of MIA synthesis seems to be an early event in carcinogenesis, taking into account that all in situ tumors express it. The objective of this study was to assess the significance of increased serum MIA concentration in MM patients with no metastases at primary diagnoses. Materials and methods Between 2008-2012 we have collected 200 blood samples from 150 patients with non-metastatic MM and 50 healthy donors. The patients were staged according to TNM classification 2009 as follows: 28 in stage I, 72 in stage II and 50 in stage III. The blood was withdrawn after the primary tumor excision and before any other treatment. MIA was measured by a high sensitivity ELISA method, with a kit produced by Roche Diagnostics. Using the ROC curve, MIA cut-off value was set at 9.4 ng/ml [4]. Results We estimated overall survival (OS) and disease free survival (DFS) for the entire lot and for each stage separately, according to MIA cut-off level. The length of follow-up was 44 month, from the moment of MIA measurement. Univariate Cox regression suggested that patients with an increased MIA serum concentration had a three times higher risk of relapse (HR=3.3895) and death (HR = 2.7597) than patients with values under the calculated threshold (p=0.000). More important is that MIA keeps statistical significance in multivariate analyses, predicting risk of death or relapse after corrections for clinical stage. Conclusions In our study, MM patients with a MIA serum concentration above 9.4 ng/ml had a worse DFS (p=0.0109) and OS (p=0.0009) than patients with values below 9.4 ng/ml. We consider that MIA serum concentration is a valuable prognostic factor and could become a tool for selecting patients at risk for developing metastases rendering them eligible for neoadjuvant treatment.


Journal of Biotechnology | 2017

One Health and advanced biotechnology

Nicolae Manolescu; Emilia Balint; Sabin Cinca; Calin Cristian Chirila

1 “Prof. Dr. Alex.Trestioreanu” Oncological Institute, Bucharest, Romania 2 Faculty of Veterinary Medicine, University of Agronomic Sciences and Veterinary Medicine, Bucharest, Romania 3 One Health – New Medical Concept Association, Bucharest, Romania Corresponding author: Nicolae Manolescu “Prof. Dr. Alex.Trestioreanu” Oncological Institute, Bucharest, Romania. E-mail:[email protected] Abstract


Journal of Translational Medicine | 2015

Simultaneous determination of two serum tumor markers in assessing malignant melanoma patients

Angela Sandru; Silviu Voinea; Eugenia Panaitescu; Madalina Bolovan; Adina Stanciu; Sabin Cinca; Alexandru Blidaru

Background The incidence of cutaneous malignant melanoma (MM) continues to raise despite extensive prevention programs. If localized disease can be cured, the prognosis of metastatic melanoma is grim. Therefore, reliable methods to detect patients at risk for disease progression are sought. Field of tumor markers has captured attention because it allows the first steps toward personalized medicine. A positive tumor marker has a limited ability to correctly detect all sick people, so it was proposed to simultaneously measure several markers in order to improve their performance [1,2]. S100 and Melanoma Inhibitory Activity (MIA) are most frequently used for monitoring MM patients. Both proteins have a high specificity and their expression correlates with body tumor burden [3].


Journal of Translational Medicine | 2015

Melanoma Inhibitory Activity and regional lymph node status in malignant melanoma patients

Angela Sandru; Silviu Voinea; Eugenia Panaitescu; Madalina Bolovan; Adina Stanciu; Sabin Cinca; Alexandru Blidaru

Background For many cancers, and malignant melanoma (MM) makes no exception, regional lymph node (RLN) status is decisive for subsequent patients’ outcome. But particularly for MM, stage III comprises a very heterogeneous group of patients, from those with microscopic invasion diagnosed by sentinel node (SN) biopsy to those with matted nodes. Correct staging of patients with clinically free RLN requires SN biopsy. Because this is an invasive maneuver, various substitutes were searched. Thus, in literature there are conflicting references to a possible link between Melanoma Inhibitory Activity (MIA) serum concentration and SN status [1,2]. MIA, a protein secreted by malignant melanocytes into the extracellular space, blocks the melanoma cells attachment to fibronectin and laminin. Thus MIA increases malignant cells mobility and promotes local invasion and metastasis [3]. In this context, we sought a connection between RLN status and MIA serum concentration in our group of patients.


Archive | 2005

Deuterium Depleted Water (Ddw) Using As Adjuvant In Cancer Therapy For Cytostatics Toxicity Reducing

Nicolae Manolescu; Serban Constantin Valeca; Rodica Anghel; Ion Balanescu; Rodin Traicu; Dumitru Marculescu; Ioan Stefanescu; Marieta Panait; Emilia Balint; Ioan Encut; Manuella Militaru; Aneta Pop; Sabin Cinca; Virgiliu Comisel; Viorel Fugaru; Corneliu Mateescu; Iuliana Gruia; Victoria Moraru; Monica Nistoroiu; Daniela Begu; Iolanda Dumitrescu; Maria Ghita


Journal of Biotechnology | 2018

Identifying the melanoma patients with high risk for metastasis

Madalina Bolovan; Sabin Cinca; Antonela Busca; Adina Stanciu; Eugenia Panaitescu; Angela Sandru; Silviu Voinea


Journal of Biotechnology | 2017

Concomitant determination of MIA and S100 proteins as prognostic factors in cutaneous malignant melanoma

Madalina Bolovan; Silviu Voinea; Eugenia Panaitescu; Adina Stanciu; Antonela Busca; Sabin Cinca; Angela Sandru


Journal of Biotechnology | 2016

Molecular and ultrastructural aspects in invasive mammary carcinoma

Corina Elena Mihalcea; Liliana Puiu; Ana Maria Morosanu; Daniela Murarasu; Silviu Voinea; Sabin Cinca; Nicolae Mirancea


Journal of Biotechnology | 2016

KRAS, BRAF and TP53 mutations in Romanian colorectal cancer patients

Daniela Murarasu; Liliana Puiu; Corina Elena Mihalcea; Sabin Cinca; Laurentiu Simion


Archive | 2015

TRENDS IN CANCER INCIDENCE AND MORTALITY - COMPARATIVE DATA WORLDWIDE, EUROPEAN UNION, AND ROMANIA

Nicolae-Dan Straja; Marieta Panait; Antonela Busca; Sabin Cinca

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Silviu Voinea

Carol Davila University of Medicine and Pharmacy

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Angela Sandru

Carol Davila University of Medicine and Pharmacy

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Eugenia Panaitescu

Carol Davila University of Medicine and Pharmacy

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Alexandru Blidaru

Carol Davila University of Medicine and Pharmacy

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Emilia Balint

University of Agricultural Sciences

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Nicolae Manolescu

University of Agricultural Sciences

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Aneta Pop

University of Agronomic Sciences and Veterinary Medicine of Bucharest

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