Base Preferences in Non-Templated Nucleotide Incorporation by MMLV-Derived Reverse Transcriptases.docVIP
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Base Preferences in Non-Templated Nucleotide Incorporation by MMLV-Derived Reverse Transcriptases
Base Preferences in Non-Templated Nucleotide
Incorporation by MMLV-Derived Reverse Transcriptases
Pawel Zajac , Saiful Islam, Hannah Hochgerner , Peter L?nnerberg, Sten Linnarsson
¤a ¤b *
Laboratory for Molecular Neurobiology, Department of Medical Biochemistry and Biophysics, Karolinska Institutet, Stockholm, Sweden
Abstract
Reverse transcriptases derived from Moloney Murine Leukemia Virus (MMLV) have an intrinsic terminal transferase
activity, which causes the addition of a few non-templated nucleotides at the 3′ end of cDNA, with a preference for
cytosine. This mechanism can be exploited to make the reverse transcriptase switch template from the RNA
molecule to a secondary oligonucleotide during first-strand cDNA synthesis, and thereby to introduce arbitrary
barcode or adaptor sequences in the cDNA. Because the mechanism is relatively efficient and occurs in a single
reaction, it has recently found use in several protocols for single-cell RNA sequencing. However, the base preference
of the terminal transferase activity is not known in detail, which may lead to inefficiencies in template switching when
starting from tiny amounts of mRNA. Here, we used fully degenerate oligos to determine the exact base preference
at the template switching site up to a distance of ten nucleotides. We found a strong preference for guanosine at the
first non-templated nucleotide, with a greatly reduced bias at progressively more distant positions. Based on this
result, and a number of careful optimizations, we report conditions for efficient template switching for cDNA
amplification from single cells.
Citation: Zajac P, Islam S, Hochgerner H, L?nnerberg P, Linnarsson S (2013) Base Preferences in Non-Template
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