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Nucleic acid amplification

  • US 10,036,060 B2
  • Filed: 10/29/2014
  • Issued: 07/31/2018
  • Est. Priority Date: 12/22/2000
  • Status: Active Grant
First Claim
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1. A method of amplifying RNA sequences complementary to, or present in, one or more than one target polynucleotide that is single stranded or made single stranded, comprising:

  • a) forming double stranded cDNA templates containing sequences present in said one or more than one target polynucleotide by;

    i) annealing said one or more than one target polynucleotide with a first oligonucleotide comprising an anchor sequence and a primer operably linked to a promoter region to form a first complex, wherein a molar ratio of primers to single stranded target polynucleotide is from about 500;

    1 to about 8000;

    1,ii) synthesizing one or more than one first strand cDNA by reverse transcription of said first complex,iii) degrading first oligonucleotides not used in i) or ii) above with exonuclease activity,iv) annealing said one or more than one first strand cDNA, after denaturing the hybrid(s) of single stranded target polynucleotide and cDNA or degrading the single stranded target polynucleotide from said hybrid(s), with a plurality of second oligonucleotides comprising a random primer region comprising at least about six random nucleotides to form a population of second complexes, andv) forming one or more than one double stranded cDNA templates from said population of second complexes with DNA dependent DNA polymerase activity;

    b) transcribing said one or more than one double stranded cDNA templates with an RNA polymerase capable of initiating transcription via said promoter region to produce amplified RNA (aRNA) containing sequences complementary to said one or more than one target polynucleotide;

    c) forming additional double stranded DNA templates from said aRNA by;

    i) annealing said aRNA with a third oligonucleotide comprising a primer region operably linked to a promoter region to form a third complex,ii) synthesizing the first strand of said additional DNA template by reverse transcription of said third complex to produce an aRNA/DNA hybrid,iii) annealing said first strand of additional DNA template, after denaturing the aRNA/DNA hybrid or degrading the aRNA from said hybrid, with said first oligonucleotide to form a population of fourth complexes, andiv) forming additional double stranded DNA templates from said population of fourth complexes with DNA dependent DNA polymerase activity; and

    d) transcribing said additional DNA templates with an RNA polymerase capable of initiating transcription via the promoter region of said first oligonucleotide to produce amplified RNA (aRNA) containing sequences complementary to said one or more than one target polynucleotide or via the promoter region of said third oligonucleotide to produce aRNA containing sequences present in said one or more than one target polynucleotide.

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