Boron-containing nucleic acids. 2. Synthesis of oligodeoxynucleoside boranophosphates

Sood, Anup; Shaw, Barbara Ramsay; Spielvogel, Bernard F.

doi:10.1021/ja00180a066

Cited by 154 publications

(82 citation statements)

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“…The difference in T m s of cPNAs 2 and 4 is more pronounced when they are hybridized with oligodeoxynucleotides in accord with theory (25). Thus with the oligonucleotide (dA) 10 , cPNA 2 gave a T m of 61ЊC, whereas the cPNA 4 gave a broader melting curve with a T m of approximately 42ЊC. These observations suggest that where the opportunity for cooperative binding does not exist then the cPNA 2 does bind more effectively than cPNA 4 to a complementary oligonucleotide sequence.…”

Section: Resultssupporting

confidence: 69%

Hybridization Studies with Chiral Peptide Nucleic Acids

Lowe

Vilaivan

Westwell

1997

Bioorganic Chemistry

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Section: Resultssupporting

confidence: 69%

Hybridization Studies with Chiral Peptide Nucleic Acids

Lowe

Vilaivan

Westwell

1997

Bioorganic Chemistry

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“…[1][2][3][4][5] To a great extent, these modifications have focused on replacing the phosphodiester group by phosphodiester mimics, such as phosphorothioate, [6] methylphosphate, [7] phosphoramidates, [8] boranophosphate, [9] alkylphosphotriesters, [10] phosphorodithioate, [11] phosphonomethyl, [12] propynes, [13] diene, [14] phosphonoformate, [15] and other groups. [16] The phosphate-modified ODNs have been used as inhibitors of gene expression, [1] viral enzymes, [2,3] in vitro messenger-RNA translation, [4] and sequence-specific DNA binding proteins.…”

Section: Yousef Ahmadibeni and Keykavous Parang*mentioning

confidence: 99%

Synthesis and Evaluation of Modified Oligodeoxynucleotides Containing Diphosphodiester Internucleotide Linkages

Ahmadibeni¹,

Parang²

2007

Angew Chem Int Ed

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Build a bridge: Oligodeoxynucleotides (ODNs) containing diphosphodiester bridges were synthesized by a solid‐phase synthesis strategy. Modified ODNs formed stable duplexes with complementary modified and unmodified nucleic acid sequences. The modified oligomers were resistant to degradation by DNase I and 3′‐exonuclease I under conditions in which unmodified ODNs were degraded. B=T, A, G, or C.

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“…[70] Thus, 2Ј-and 3Ј-oxygen functionalities in the uridine 13 were activated with dibutyltin oxide yielding the intermediate 2Ј,3Ј-O,O-dibutylstannyleneuridine (14). [71] Alkylation of 14 with propargyl bromide gave a mixture of 2Ј-O-(3-prop-1-ynyl)uridine (15a) and 3Ј-O-(3-prop-1-ynyl)uridine (15b).…”

Section: Containing Oligonucleotidesmentioning

confidence: 99%

Boron Clusters − A New Entity for DNA‐Oligonucleotide Modification

Leśnikowski¹

2003

Eur J Org Chem

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The carboranyl cluster is a new and versatile modifying entity for nucleotides and nucleic acids. Three types of carboranyl (−C 2 B 10 H 11 ) group-containing DNA-oligonucleotides are described: (1) CBMP-oligonucleotides, consisting of the carborane cage within an internucleotide linkage; (2) CDUoligonucleotides, containing the carborane cage attached to a nucleobase; and (3) 2Ј-CBM-oligonucleotides, with the carborane cage linked to a sugar residue at the 2Ј position. The method of synthesis and the physicochemical and biochemical features of these novel modifications are discussed, together with structure−property relationships. The carboranyl cluster-containing oligonucleotides form a crossover between (carba)borane chemistry and molecular

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Boron-containing nucleic acids. 2. Synthesis of oligodeoxynucleoside boranophosphates

Cited by 154 publications

References 0 publications

Hybridization Studies with Chiral Peptide Nucleic Acids

Hybridization Studies with Chiral Peptide Nucleic Acids

Synthesis and Evaluation of Modified Oligodeoxynucleotides Containing Diphosphodiester Internucleotide Linkages

Boron Clusters − A New Entity for DNA‐Oligonucleotide Modification

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