ABSTRACT
In the present paper, for the first time, the integrated three-electrode screen-printed sensor with in situ plated bismuth film carbon working electrode was applied for the ultratrace determination of thallium(I) (Tl(I)). Under optimized conditions extremely low limits of detection were reached, 8.47â¯×â¯10-10 and 6.71â¯×â¯10-12â¯molâ¯L-1 for the deposition times of 60â¯s and 300â¯s, respectively. The influences of foreign metal ions and surfactants on the voltammetric signal of thallium in natural samples were minimized using 1â¯×â¯10-5â¯molâ¯L-1 EDTA and Amberlite XAD-7 resin added to the buffer solution (CH3COONH4, CH3COOH and NH4Cl) of pHâ¯=â¯4.6⯱â¯0.1. The developed voltammetric method with integrated three-electrode screen-printed sensor was validated with use of certified reference materials (surface, rain and natural water) and can be in future applied to field analyses of Tl(I).
ABSTRACT
At least one of ten patients with ovarian cancer is estimated to develop their tumor because of heredity with the breast and ovarian cancer syndrome due to mutations in the BRCA1 and BRCA2 genes and hereditary nonpolyposis colorectal cancer (HNPCC) being the major genetic causes. Cancer at young age is a hallmark of heredity, and ovarian cancers associated with HNPCC have been demonstrated to develop at a particularly early age. We used the Swedish Cancer Registry to identify a population-based series of 98 invasive epithelial ovarian cancers that developed before 40 years. Mucinous and endometrioid cancers were overrepresented and were diagnosed in 27% and 16% of the tumors, respectively. Immunostaining using antibodies against MLH1, PMS2, MSH2, and MSH6 was used to assess the mismatch-repair status and revealed loss of expression of MLH1/PMS2 in two cases, loss of MSH2/MSH6 in one case, and loss of MSH6 only in three tumors. A microsatellite instability-high phenotype was verified in five of six tumors. Based on the identified mutations and family history of cancer, several of these individuals are likely to be affected by HNPCC. We conclude that although the causes of the vast majority of epithelial ovarian cancer at young age are unknown, HNPCC should be considered because of the high risk of metachronous colorectal cancer in the individual and the possibility of preventing additional cancers in the family through control programs.
Subject(s)
DNA Mismatch Repair , Ovarian Neoplasms/genetics , Adult , Age Factors , Colorectal Neoplasms, Hereditary Nonpolyposis/genetics , DNA Repair Enzymes/deficiency , DNA Repair Enzymes/genetics , DNA Repair Enzymes/metabolism , Female , Humans , Ovarian Neoplasms/enzymology , Ovarian Neoplasms/pathologyABSTRACT
Eleven Polish and Hungarian isolates of Infectious bursal disease virus (IBDVs) obtained in the 70/80s (early IBDV) and in the 90s (recent IBDV) were characterized in an Antigen-Capture-ELISA with a panel of neutralizing monoclonal antibodies (Mabs), and by nucleotide sequencing of the VP2 variable domain (vVP2). The viruses were compared with reference IBDV strains, among others with Faragher 52/70 (F52/70, classical, isolated 1970), 89163 (typical very virulent-vvIBDV, isolated 1989) and 91168 (antigenically modified vvIBDV, isolated 1991). Only one of the early isolates (Hungarian strain P1) proved antigenically and genetically similar to F52/70. Other early isolates exhibited no reactivity versus Mabs 3, 4, 5 and/or 8 and had a common previously unrecognized combination of amino acid changes in vVP2. The recent isolates all proved antigenically and genetically related to typical vvIBDV strain 89163, except the Polish isolate 93/35 which proved related to the 91168 strain although no epidemiological relationship had been documented between these viruses in the field. Phylogenetic analysis confirmed that the non-P1 early IBDVs represent a previously unrecognized group among serotype 1 IBDVs. It is discussed whether these early isolates are derivatives of the F52/70-like viruses that might still be present in the field, or whether they represent early IBDV strains that might have been present prior to and progressively replaced by the F52/70-like viruses, as the latter have been replaced by vvIBDVs in the late eighties.
