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Last Updated: April 16, 2024

Details for Patent: 7,625,873


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Title:Antisense antibacterial method and compound
Abstract: A method and antisense compound for inhibiting the growth of pathogenic bacterial cells are disclosed. The compound contains no more than 12 nucleotide bases and has a targeting nucleic acid sequence of no fewer than 10 bases in length that is complementary to a target sequence containing or within 10 bases, in a downstream direction, of the translational start codon of a bacterial mRNA that encodes a bacterial protein essential for bacterial replication. The compound binds to a target mRNA with a T.sub.m of between 50.degree. to 60.degree. C. The relatively short antisense compounds are substantially more active than conventional antisense compounds having a targeting base sequence of 15 or more bases.
Inventor(s): Geller; Bruce L. (Corvallis, OR), Deere; Jesse D. (Davis, CA), Iversen; Patrick L. (Corvallis, OR), Weller; Dwight D. (Corvallis, OR)
Assignee: AVI BioPharma, Inc. (Corvallis, OR)
Filing Date:May 10, 2006
Application Number:11/432,216
Claims:1. A method of inhibiting the growth of Escherichia coli, Salmonella typhimurium, or Yersinia pestis pathogenic bacterial cells, comprising exposing the bacterial cells to a growth-inhibiting amount of an antisense oligonucleotide compound, composed of morpholino subunits and phosphorus-containing intersubunit linkages joining a morpholino nitrogen of one subunit to a 5' exocyclic carbon of an adjacent subunit, and having: (i) no more than 12 nucleotide bases, (ii) a targeting nucleic acid sequence of no fewer than 10 bases in length that is complementary to a target sequence containing or within 10 bases, in a downstream direction, of the translational start codon in SEQ ID NO: 2; and (iii) a T.sub.m, when hybridized with the target sequence, between 50.degree. to 60.degree. C.; wherein said morpholino subunits in the oligonucleotide compound are joined by a combination of (a) uncharged phosphorodiamidate linkages, in accordance with structure I, ##STR00003## where Y.sub.1.dbd.O, Z=O, Pj is a purine or pyrimidine base-pairing moiety effective to bind, by base-specific hydrogen bonding, to a base in a polynucleotide, and X is amino or alkyl amino, including dialkylamino; and (b) cationic phosphorodiamidate linkages in accordance with structure I, where Y.sub.1.dbd.O, Z=O, and P.sub.j are as defined above, and X is 1-piperazino; and wherein said cationic linkages make up no more than about half the total number of linkages.

2. The method of claim 1, wherein X in said uncharged linkages is N(CH.sub.3).sub.2.

3. The method of claim 1, wherein the oligonucleotide compound to which the cells are exposed has a targeting sequence that is complementary to a target sequence containing the translational start codon of the bacterial mRNA.

4. The method of claim 1, wherein the oligonucleotide compound to which the cells are exposed has a targeting sequence that is complementary to a target sequence that is within 10 bases, in a downstream direction, of the translational start codon of the bacterial mRNA.

5. The method of claim 1, wherein the oligonucleotide compound to which the cells are exposed contains only 11 bases, and its nucleic acid sequence is completely complementary to the mRNA target sequence.

6. The method of claim 1, for use in inhibiting a bacterial Escherichia coli, Salmonella typhimurium, or Yersinia pestis infection in a mammalian subject, wherein said exposing includes administering said compound in a therapeutically effective amount.

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