Inclisiran: A New Promising Agent in the Management of Hypercholesterolemia

Kosmas, Constantine E.; Estrella, Alba Munoz; Sourlas, Andreas; Silverio, Delia; Elizabeth, Hilario; Montan, Peter D; Guzman, Eliscer

doi:10.3390/diseases6030063

Cited by 86 publications

(60 citation statements)

References 26 publications

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“…Inclisiran is a long-acting small interfering RNA (siRNA) molecule directed against PCSK9, and it has been shown to significantly decrease hepatic production of PCSK9 and cause a marked reduction in LDL-C levels. 37 This agent is not licensed as yet and has not been proven to reduce cardiovascular outcomes, as of now. However, inclisiran appears very promising and, in the future, if approved, its use may lead to a significant improvement in adherence and compliance due to its very infrequent, 6-monthly dosing intervals.…”

Section: Discussionmentioning

confidence: 99%

Patient adherence, compliance, and perspectives on evolocumab for the management of resistant hypercholesterolemia

Kosmas¹,

Silverio²,

Ovalle³

et al. 2018

PPA

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Evolocumab is a PCSK9 inhibitor which is administered subcutaneously, and when added to statin therapy it has been shown to cause a significant incremental LDL-C reduction, leading to a reduction of cardiovascular risk. Evolocumab has a favorable side effect profile, and its self-administration at home appears to be safe and effective with the appropriate training and instructions from a health care provider. Current studies are showing encouraging results regarding adherence to evolocumab in real-life settings, and adherence rates to evolocumab appear to be better than those to statins. However, further larger studies are needed for a more definitive assessment of the short- and long-term patient adherence rates to evolocumab. In addition, reductions in the price of evolocumab may also be necessary to improve cost-effectiveness of the drug.

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Section: Discussionmentioning

confidence: 99%

Patient adherence, compliance, and perspectives on evolocumab for the management of resistant hypercholesterolemia

Kosmas¹,

Silverio²,

Ovalle³

et al. 2018

PPA

Self Cite

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“…These drugs are lumasiran, vutrisiran, givosiran, and inclisiran, which are agents against primary hyperoxaluria type 1, transthyretin mediated amyloidosis, acute hepatic porphyria, and hypercholesterolemia, respectively. 1,[28][29][30][31] Like the mentioned siRNAs, there are a huge group of miRNAs and antagomirs that are already identified as remarkably stimulators of osteoblast/osteocytic lineage differentiation, proliferation, and survival. In Table 1, we show the most studied miRNAs and antagomirs in relation to bone signaling pathways, their targets, and their final response to bone turnover.…”

Section: Therapeutic Nucleic Acids and Their Mechanismmentioning

confidence: 99%

Signaling pathways of nucleic acids for bone healing: A review

Ruggieri¹,

Feldman²

2020

PPIJ

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“…Inclisiran is composed of one 2′-deoxy, eleven 2′-fluoro-, and thirty-two 2′-O-methyl-modified nucleotides, and a triantennary N-acetylgalactosamine (GalNAc) that is conjugated to the 3′-end of the passenger strand. The asialoglycoprotein receptor recognizes the GALNAc inhibiting the uptake of Inclisiran, resulting in the reduction of PCSK9 mRNA by 70% [113]; (2) Antisense Oligonucleotides (ASOs) inhibit the PCSK9 mRNA protein synthesis decreasing intra and extracellular protein levels. SPC5001, the clinical grade product of this approach, is 14 base oligonucleotide relying on locked nucleic acid technology with higher binding and specificity for PCSK9 mRNA [12]; (3) it has been proposed to block the PCSK9 expression by targeting the ribosomal complex using biologically active small molecules, in this way PF-06446846 (PF846) a small active molecule has been developed that directly inhibits the translation of PCSK9 by stalling the 80S ribosome in codon 34.…”

Section: Article Highlightsmentioning

confidence: 99%

“…In a follow-up, Orion-1 was a phase 2, double-blind, placebo-controlled, dose-finding study in 501 patients with a high risk of CVD with LDL-C levels > 70 mg/dL in the presence of atherosclerotic history or LDL-C > 100 mg/dL in the absence of risk of ASCVD history. The studies report on day 180 a significant reduction of LDL-C up to 50 mg/dL level that was obtained with two doses of 300 mg inclisiran at 48% of patients [113]. The ORION-7 study evaluated the effect of inclisiran on pharmacokinetics (PK) and pharmacodynamics (PD) in individuals with different degrees of renal impairment.…”

Section: Small Interfering Rna (Inclisiran)mentioning

confidence: 99%

Progress and prospects of biological approaches targeting PCSK9 for cholesterol-lowering, from molecular mechanism to clinical efficacy

Malvandi

Canclini

Alliaj

et al. 2020

Expert Opinion on Biological Therapy

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Introduction: Cardiovascular disorders are one of the leading causes of mortality and morbidity worldwide. Recent advances showed a promising role of proprotein convertase subtilisin/kexin type 9 (PCSK9) as a critical player in regulating plasma LDL levels and lipid metabolism. Areas covered: This review addresses the molecular functions of PCSK9 with a vision on the clinical progress of utilizing monoclonal antibodies and other biological approaches to block PCSK9 activity. The successful clinical trials with monoclonal antibodies are reviewed. Recent advances in (pre)clinical trials of other biological approaches, such as small interfering RNAs, are also discussed. Expert opinion: Discovery of PCSK9 and clinical use of its inhibitors to manage lipid metabolism is a step forward in hypolipidaemic therapy. A better understanding of the molecular activity of PCSK9 can help to identify new approaches in the inhibition of PCSK9 expression/activity. Whether if PCSK9 plays a role in other cardiometabolic conditions may provide grounds for further development of therapies.

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Inclisiran: A New Promising Agent in the Management of Hypercholesterolemia

Cited by 86 publications

References 26 publications

Patient adherence, compliance, and perspectives on evolocumab for the management of resistant hypercholesterolemia

Patient adherence, compliance, and perspectives on evolocumab for the management of resistant hypercholesterolemia

Signaling pathways of nucleic acids for bone healing: A review

Progress and prospects of biological approaches targeting PCSK9 for cholesterol-lowering, from molecular mechanism to clinical efficacy

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