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2. ChIP sequencing - Wikipedia

   en.wikipedia.org/wiki/ChIP_sequencing

   ChIP-sequencing, also known as ChIP-seq, is a method used to analyze protein interactions with DNA. ChIP-seq combines chromatin immunoprecipitation (ChIP) with massively parallel DNA sequencing to identify the binding sites of DNA-associated proteins. It can be used to map global binding sites precisely for any protein of interest.

3. Carlson curve - Wikipedia

   en.wikipedia.org/wiki/Carlson_Curve

   The Carlson curve is a term to describe the rate of DNA sequencing or cost per sequenced base as a function of time. [1] It is the biotechnological equivalent of Moore's law. Carlson predicted that the doubling time of DNA sequencing technologies (measured by cost and performance) would be at least as fast as Moore's law. [2]

4. Chromatin immunoprecipitation - Wikipedia

   en.wikipedia.org/wiki/Chromatin_immunoprecipitation

   The cost and accessibility of ChIP-seq is a major disadvantage, which has led to the more predominant use of ChIP-chip in laboratories across the world. [2] This photo compares the efficacy of the two experimental techniques, ChIP-seq and ChIP-chip. Table 1 Advantages and disadvantages of NChIP and XChIP

5. Hi-C (genomic analysis technique) - Wikipedia

   en.wikipedia.org/wiki/Hi-C_(genomic_analysis...

   Any platform that can allow for the ligated fragments to be sequenced across the NheI junction (Roche 454) or by paired-end or mate-paired reads (Illumina GA and HiSeq platforms) would be suitable for Hi-C. [4] Before high-throughput sequencing, the quality of the library should be verified using Sanger sequencing, wherein the long sequencing ...

6. DNA sequencing - Wikipedia

   en.wikipedia.org/wiki/DNA_sequencing

   Sequencing by ligation (SOLiD sequencing) 50+35 or 50+50 bp: 99.9%: 1.2 to 1.4 billion: 1 to 2 weeks: $60–130: Low cost per base. Slower than other methods. Has issues sequencing palindromic sequences. [101] Nanopore Sequencing: Dependent on library preparation, not the device, so user chooses read length (up to 2,272,580 bp reported [102 ...

7. ChIP-on-chip - Wikipedia

   en.wikipedia.org/wiki/ChIP-on-chip

   The cost of the DNA microarrays is often a limiting factor to whether a laboratory should proceed with a ChIP-on-chip experiment. Another limitation is the size of DNA fragments that can be achieved. Most ChIP-on-chip protocols utilize sonication as a method of breaking up DNA into small pieces.

8. Chromosome conformation capture - Wikipedia

   en.wikipedia.org/wiki/Chromosome_conformation...

   Hi-C uses high-throughput sequencing to find the nucleotide sequence of fragments [2] [22] and uses paired end sequencing, which retrieves a short sequence from each end of each ligated fragment. As such, for a given ligated fragment, the two sequences obtained should represent two different restriction fragments that were ligated together in ...

9. Personal genomics - Wikipedia

   en.wikipedia.org/wiki/Personal_genomics

   Personal genomics or consumer genetics is the branch of genomics concerned with the sequencing, analysis and interpretation of the genome of an individual. The genotyping stage employs different techniques, including single-nucleotide polymorphism (SNP) analysis chips (typically 0.02% of the genome), or partial or full genome sequencing.