3 research outputs found

    Importance of microsatellite instability determination as genetic marker in colorectal cancer

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    UVOD: Nastanak i klinički tok kolorektalnog karcinoma (CRC) rezultat je mnogobrojnih genetskih faktora i faktora sredine, i njihovih interakcija. Mikrosatelitna nestabilnost (MSI) je genetski marker koji se koristi u dijagnostici Lynch sindroma. U sporadičnim formama CRC proučava se prognostički značaj ovog molekularnog fenomena. CILJ: Ispitivanje prognostičkog značaja mikrosatelitne nestabilnosti kao genetskog markera u CRC, kliničkih i patohistoloÅ”kih parametara koji ukazuju na MSI u CRC. METOD: U istraživanje je uključeno 150 pacijenata muÅ”kog i ženskog pola sa kolorektalnim karcinomom koji su hospitalizovani radi operativnog lečenja na Klinici za digestivnu hirurgiju, Kliničkog Centra Srbije od 2006. do 2010. godine. U operativnom uzorku testirana je MSI, Pentaplex PCR metodom sa pet obeleženih mononukleotidnih markera (BAT25, BAT26, NR-21, NR-22 i NR-24). Grupu je podeljena na osnovu MSI statusa: MSI-H grupa (nestabilnost u viÅ”e od tri markera) i MSS/L grupa (nestabilnost u manje od tri markera). Klinički i patohistoloÅ”ki parametri korelisani su između grupa. Pacijenti su praćeni u smislu pojave lokalnog ili udaljenog recidiva ili do smrtnog ishoda do septembra 2012. godine. REZULTATI: U MSI-H grupi bilo je 18 pacijenata, dok je u MSS/L grupi bilo 132 pacijenta. Uni i multivarijanti logistički regresioni modeli su pokazali da tumori lokalizovani u desnom kolonu sa izraženijom mucinskom produkcijom, slaba diferentovanost i ispunjenost bar jednog revidiranog Bethesda kriterijuma predstavljaju najznačajnije prediktivne parametre za MSI. Postoji značajna statistička razlika u DFS (period bez znakova recidiva bolesti; engl. disease free survival) između MSI-H i MSS/L grupa (Kaplan Meir test; p=0,048, log rank). Nije bilo statistički značajne razlike u celokupnom i bolest-specifičnom preživljavanju između grupa. ZAKLJUČAK: Mikrosatelitna nestabilnost je detektovana u 12% bolesnika sa kolorektalnim karcinomom. Kliničke i patohistoloÅ”ke karakteristike tumora koje ukazuju na MSI-H fenotip su lokalizacija u desnom kolonu, mucinska produkcija, slabija diferentovanost. Mikrosatelitna nestabilnost predstavlja prognostički faktor koji je povezan sa manjom stopom pojave recidiva (lokalnih ili udaljenih metastaza) kod pacijenata sa kolorektalnih karcinoma u I, II i III stadijumu bolesti, ali ne utiče na bolest-specifično i celokupno preživljavanje pacijenata sa CRC.INTRODUCTION: Colorectal cancer (CRC) is the result of interaction between numerous genetic and environmental factors. Microsatellite instability (MSI) is a genetic marker that can be useful in the diagnosis of Lynch syndrome and may have a prognostic significance in sporadic colorectal cancer. OBJECTIVE: The aim of present study was to test the prognostic significance of microsatellite instability as genetic marker in CRC, to examine the clinical and histological parameters that indicate on MSI in CRC. METHOD: The study included 150 patients with colorectal cancer, who were hospitalized for surgical treatment at the Department of Digestive Surgery, Clinical Center of Serbia since 2006. to 2010. CRC samples were tested for MSI by Pentaplex PCR with five mononucleotide, microsatellite markers (BAT25, BAT26, NR-21, NR-22 and NR-24). The group was divided acording to the MSI status: MSI-H group (instability in more than three markers) and MSS/L group (instability in less than three markers). Clinical and histopathological parameters were correlated between the groups. Patients were followed up for possible local or distant disease recurrence or up to death to September 2012. RESULTS: 18 patients had MSI-H CRC, and they represented MSI-H group while in the MSS/L group comprised of the remaining 132 patients. Uni and multivariate logistic regression models showed that primary lesions located in the right colon with prominent mucin production, poor differentiation, and the fulfillment of at least one of the revised Bethesda criteria were the most important predictive parameters for MSI. There was a statistically significant difference in DFS (period without any recurrence; Disease Free Survival) between MSI-H and MSS/L group (Kaplan Meir test, p = 0.048, log rank). There was no statistically significant difference in overall and disease-specific survival between groups. CONCLUSION: Microsatellite instability was detected in 12% of patients with colorectal cancer. Clinical and pathological characteristics of CRC that show MSI-H phenotype are localization the right colon, prominent mucin production and poor differentiation. MSI represents a prognostic factor associated with a lower rate of recurrence (local or distant metastases) in patients with colorectal cancer in the first, second and third stage of the disease, but does not affect the disease-specific and overall survival in patients with CRC

    Procena ekoloŔkog rizika u funkciji zaŔtite životne sredine

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    This paper proposes an appropriate methodology for ecological risk assessment. The methodology has been applied in the region of Boka Kotorska Bay (Bay), Montenegro. The emphasis of the research is on the analysis of the impact of various stressors on the ecological components of Bay. The consequences of that impact can be seen in an increased level of eutrophication of water environment, mostly through the influence of nitrogen and its compounds. The actual research at/about the region of Boka Kotorska Bay was performed in the period of 2008. The study emphasized the importance of the acquisition, processing and analysis of various ecologically related data for more efficient monitoring and management of the environment. The suggested methodology of the ecological risk assessment is, therefore, a remarkable scientific and expert contribution in the area of environmental protection in our country and in general.U radu je predstavljena primena metodologije procene ekoloÅ”kog rizika. Metodologija je primenjena na primeru Bokokotorskog zaliva (Zaliv). Istraživanjem je razmatrana procena uticaja većeg broja stresora na ekoloÅ”ke komponente Zaliva. Posledice ovih uticaja ispoljene su kroz povećan stepen eutrofikacije vodene sredine i dovode se u vezu sa koncentracijom azotnih jedinjenja (nitrata i nitrita) Konkretna merenja vrÅ”ena su u 2008. godini. Istraživanjem je posebno ukazano na značaj razvoja sistema prikupljanja i obrade ekoloÅ”kih i drugih informacija radi efikasnijeg upravljanja životnom sredinom datog prostora. Primenjena metodologija procene ekoloÅ”kog rizika trebalo bi da u naučnom i stručnom pogledu predstavlja doprinos u oblasti zaÅ”tite životne sredine,kako kod nas, tako i u svetu

    Oral squamous cell carcinoma detection by salivary biomarkers in a Serbian population

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    Early detection of oral squamous cell cancer (OSCC) is the key to improve the low 5-year survival rate. Using proteomic and genomic technologies we have previously discovered and validated salivary OSCC markers in American patients. The question arises whether these biomarkers are discriminatory in cohorts of different ethnic background. Six transcriptome (DUSP1, IL8, IL1B, OAZ1, SAT1, and S100P) and three proteome (IL1B, IL8, and M2BP) biomarkers were tested on 18 early and 17 late stage OSCC patients and 51 healthy controls with quantitative PCR and ELISA. Four transcriptome (IL8, IL1B, SAT1, and S100P) and all proteome biomarkers were significantly elevated (p lt 0.05) in OSCC patients. The combination of markers yielded an AUC of 0.86, 0.85 and 0.88 for OSCC total, T1-T2, and T3-T4, respectively. The sensitivity/specificity for OSCC total was 0.89/0.78, for T1-T2 0.67/0.96, and for T3-T4 0.82/0.84. In conclusion, seven of the nine salivary biomarkers (three proteins and four mRNAs) were validated and performed strongest in late stage cancer. Patient-based salivary diagnostics is a highly promising approach for OSCC detection. This study shows that previously discovered and validated salivary OSCC biomarkers are discriminatory and reproducible in a different ethnic cohort. These findings support the feasibility to implement multi-center, multi-ethnicity clinical trials towards the pivotal validation of salivary biomarkers for OSCC detection
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