Project description:Target-enrichment baits for stony corals (Cnidaria: Anthozoa: Scleractinia)

Project description:A transcriptomic approach to resolve the sea urchin (Echinoidea, Echinodermata) phylogeny

Project description:The complete mitochondrial genome of Acanthastrea maxima (Cnidaria, Scleractinia, Lobophylliidae)

Project description:Untangling deep-sea corals systematics: description of a new family, Stephanocyathidae (Anthozoa, Scleractinia), through a genomic approach. Targeted loci

Project description:Porites lobata (Cnidaria: Scleractinia) and Cladocopium sp. (Dinoflagellata: Symbiodiniaceae) transcriptome data

Project description:LINEAR MITOCHONDRIAL GENOME IN ANTHOZOA (CNIDARIA): A CASE STUDY IN CERIANTHARIA

Project description:Coupling DNA barcodes and exon-capture to resolve the phylogeny of Turridae

Project description:This dataset consists of 39 noncancerous donor and 62 cancer patient plasma samples (including 29 patients with CRC across a total of 13 tumor types) that were analyzed with the PGDx elio plasma resolve assay. The PGDx elio plasma resolve assay is a hybrid capture approach targeting 33 genes with sequencing performed using the Illumina NextSeq with 150bp paired-end reads. The bam files provided have been adapter masked and contain duplicate reads.

Project description:Tubes of Ceriantharia (Cnidaria Anthozoa): a marine habitation. From its construction to its guests.

Project description:We applied the solution hybrid selection approach to the enrichment of CpG islands (CGIs) and promoter sequences from the human genome for targeted high-throughput bisulfite sequencing. A single lane of Illumina sequences allowed accurate and quantitative analysis of 1 million CpGs in more than 21,408 CGIs and 15,946 transcriptional regulatory regions. More than 85% of capture probes successfully yielded quantitative DNA methylation information of targeted regions. In this study, we generated genome-wide, single-base resolution DNA methylation maps in three of the most commonly used breast cancer cell lines.Differentially methylated regions (DMRs) were identified in the 5?-end regulatory regions, as well as the intra- and intergenic regions, particularly in the X chromosome among the three cell lines. The single CpG resolution methylation maps of many known tumor suppressor genes were also established in the three cell lines. Here we present a novel approach that combines solution-phase hybrid selection and massively parallel bisulfite sequencing to profile DNA methylation in targeted CGI and promoter regions. We designed 51,466 single strand DNA oligonucleotides (160-mer) which target 23,441 CGIs and the transcription start sites of 19,369 known genes in the human genome. The synthetic long DNA oligonucleotides were converted into biotinylated RNA probes for solution-phase hybridization capture of target DNA. The captured genomic DNA was treated with sodium bisulfite, amplified by PCR and sequenced using Illumina GA IIx sequencer.