Role Of The Eukaryotic Cytoskeleton Quizlet
The structure in the HCC1187 genome. A) Spectral karyotype as in [44]. Chromosomes are named A-Z and a-k based on their relative sizes as in [12]. Cytogenetic description on the karyotype is in Table S1 in File S2. B) Circos plot [45] from the HCC1187 genome: Chromosome ideograms around the outdoors, oriented clockwise pter to qter. Moving inward, the pale grey and dark grey boxes are chromosome segments observed by array painting [12] with their chromosome of origin indicated. Their parent of origin (light grey and dark grey) was deduced from the quantity of allelotypes given by PICNIC segmentation (Fig. S1 in File S1). Note that assignment of parents 1 and 2 doesn't transfer among chromosomes. Dark blue line, total copy quantity, equivalent to array CGH, from PICNIC. Red line, copy number of the minor allele; exactly where this can be zero, the genome is homozygous. Chromosome segments that share a translocation breakpoint were assumed to have precisely the same parental origin. Inner hyperlinks represent interchromosome translocations identified previously [12?14]. doi:ten.1371/journal.pone.0064991.gFigure 3. Chromosome segments in HCC1187 and their most probable state before endoreduplication. Chromosome ideograms are drawn around the outside as in Fig. 2. Outer rings are array painting segments as in Fig. 2. Inner rings are chromosome segments that must have been present just before endoreduplication. Coloured circles are different types of mutations, on the outer chromosome segment on which they were observed: AMG-337 site truncating (red), nonsynonymous (blue), little deletion (yellow), small duplication (black), expressed gene fusion (light blue). Mutations that had been on two copies of a chromosome segment probably occurred just before endoreduplication and are also shown around the inner, pre-endoreduplication genome. Dashed grey boxes on chromosome 1 and 11 indicate regions where parental origin was undetermined, because PICNIC segmentation recommended extra rearrangements had taken place. doi:10.1371/journal.pone.0064991.gduplications. The resulting image from the likely history of the karyotype almost precisely fits the recommended monosomic pattern of evolution (Fig. 1), with every single unbalanced translocation top to loss of one particular chromosome, plus some whole-chromosome losses. We next determined irrespective of whether the somatic mutations most likely occurred just before or following endoreduplication. As most loci in this genome had duplicated only once we could infer regardless of whether a mutation happened ahead of or soon after endoreduplication: in the event the mutation occurred ahead of, it will be present in two copies after the duplication, whereas when the mutation occurred right after endoreduplication, it would only be present on one particular of two copies. This classification will be incorrect if gene conversion had occurred, i.e. copying of an allele from 1 chromosome to another, but all ofthe 83 sequence-level mutations analysed beneath have been identified on only a single parent of origin, implying that gene conversion was rare or absent in this cell line, as is typical for epithelial cancers [21,22]. We placed each structural mutation just before or soon after endoreduplication, in accordance with no matter whether the translocation junction or deletion was duplicated, or involved only a single copy of a pair of participating chromosomes (Figs. 2 and 3). For the three regions of your genome that had been triplicated we assumed that one duplication had occurred at endoreduplication and yet another had occurred later.