Rapid, low-input, low-bias construction of shotgun fragment libraries by high-density in vitro transposition.
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https://www.ncbi.nlm.nih.gov/sra/SRP004087
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资源简介:
We characterize and extend a highly efficient method for constructing shotgun fragment libraries in which transposase catalyzes in vitro DNA fragmentation and adaptor incorporation simultaneously. We apply this method to sequencing a human genome and find that coverage biases are comparable to those of conventional protocols. We also extend its capabilities by developing protocols for sub-nanogram library construction, exome capture from 50 ng of input DNA, PCR-free and colony PCR library construction, and 96-plex sample indexing.
创建时间:
2015-02-09



