ABSTRACT
Alteration experiments involving intermediate level nuclear waste (ILW) glass in contact with hardened cement paste (HCP) were performed to assess its behavior under simulated repository conditions. Batch experiments were conducted at 20 °C and 50 °C in several artificial cement pore water (ACW) samples (pH from 10 to 13), in the presence of HCP (CEM-I, CEM-V and low pH), with a ratio of glass surface to volume of solution of 8000 m-1 and a ratio of mass of HCP to volume of solution of 10 g L-1. Glass alteration rates increase up to â¼4 × 10-2 g m-2 d-1 with pH in contact with HCP, notably with CEM-I. This value decreases by 2 orders of magnitude in low pH cement solution and also for residual alteration rates. The effect of calcium on glass alteration was observed, mainly in Ca(OH)2 saturated solution, with an incubation effect on the release of Si in solution. Experimental data were successfully modeled with the PhreeqC geochemical code. Glass and HCP samples were characterized via SEM/EDX and micro-Raman studies. This work showed that vitrified glass exhibits good performance in terms of low alteration rates (â¼10-4 g m-2 d-1), the absence of secondary phases, and the formation of a gel layer at the surface, when in contact with low pH conditions (in the presence or absence of low pH HCP).
ABSTRACT
BACKGROUND: The origin of melanoma has always been a debated subject, as well as the role of adjacent melanocytic naevi. Epidemiological and histopathological studies point to melanomas arising either de novo or from a naevus. OBJECTIVES: To evaluate the presence of mutations in genes from well-known melanomagenesis pathways in a large series of naevus-associated melanomas. MATERIALS AND METHODS: Sixty-one melanomas found in association with a pre-existing naevus were microdissected, after careful selection of cell subpopulations, and submitted to Sanger sequencing of the BRAF, NRAS, c-KIT, PPP6C, STK19 and RAC1 genes. Each gene was evaluated twice in all samples by sequencing or by sequencing and another confirmation method, allele-specific fluorescent polymerase chain reaction (PCR) and capillary electrophoresis detection or by SNaPshot analysis. Only mutations confirmed via two different molecular methods or twice by sequencing were considered positive. RESULTS: The majority of cases presented concordance of mutational status between melanoma and the associated naevus for all six genes (40 of 60; 66.7%). Nine cases presented concomitant BRAF and NRAS mutations, including one case in which both the melanoma and the adjacent naevus harboured V600E and Q61K double mutations. In two cases, both melanoma and associated naevus located on acral sites were BRAF mutated, including an acral lentiginous melanoma. CONCLUSIONS: To our knowledge this is the largest naevus-associated melanoma series evaluated molecularly. The majority of melanomas and adjacent naevi in our sample share the same mutational profile, corroborating the theory that the adjacent naevus and melanoma are clonally related and that the melanoma originated within a naevus.
