1997
DOI: 10.1080/07328319708006150
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Preclinical Profiling of Modified Oligonucleotides: Anticoagulation and Pharmacokinetic Properties

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Cited by 10 publications
(2 citation statements)
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“…Acute and transient toxicities from oligonucleotides include cardiovascular collapse and inhibition of clotting has been reported. These toxic responses are believed to be related to both peak plasma concentrations and the sequence lengths of the oligonucleotides (Henry et al ., ; Wallace et al ., ; Griffin et al ., ; Nicklin et al ., ). Subchronic toxicities such as immune stimulation have also been found in rodents, but are far less severe in primates (Crooke, ).…”
Section: Introductionmentioning
confidence: 97%
“…Acute and transient toxicities from oligonucleotides include cardiovascular collapse and inhibition of clotting has been reported. These toxic responses are believed to be related to both peak plasma concentrations and the sequence lengths of the oligonucleotides (Henry et al ., ; Wallace et al ., ; Griffin et al ., ; Nicklin et al ., ). Subchronic toxicities such as immune stimulation have also been found in rodents, but are far less severe in primates (Crooke, ).…”
Section: Introductionmentioning
confidence: 97%
“…29 The improvement in potency and ADME properties for second-generation ASOs in vivo over the firstgeneration chemistry has been shown to be as much as 10-fold, and, fortuitously, MOE Gapmers also benefit from a significantly reduced proinflammatory capacity, resulting in improved safety properties and a significantly increased therapeutic window (see Figure 2). [37][38][39] Although robust clinical efficacy has been achieved for several next-generation ASO and miRNA targeted therapeutics, the ADME properties are still challenges for these agents, and continued efforts to improve on the stability, potency, and cellular delivery have recently led to notable advances. The discovery and development of N-acetyl galactosamine (GalNAc)-conjugated ASOs and RNA, siRNA, have enabled the preferential delivery of these agents to hepatocytes by virtue of the affinity of GalNAc for the hepatocyte-specific asialoglycoprotein receptors.…”
Section: Rna Therapeutics Based On Antisense Principlesmentioning
confidence: 99%