BBB pathophysiology independent delivery of siRNA in traumatic brain injury

Li, Wen; Qiu, Jianhua; Li, Xiangling; Aday, Sezin; Zhang, Jingdong; Conley, Grace; Xu, Jun; Langer, Robert; Mannix, Rebekah; Karp, Jeffrey M.; Joshi, Nitin

doi:10.1101/2020.06.26.173393

Cited by 8 publications

(15 citation statements)

References 53 publications

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“…PS 80-coated PLGA NPs were developed for the efficient transport of small interfering RNA (siRNA) across the BBB in traumatic brain injury (TBI) [142] (Figure 10). siRNA-based therapeutics can mitigate disease progression in TBI treatment, but siRNA suffers from poor BBB transport.…”

Section: Ps-coated Nps For Efficient Bbb Transportmentioning

confidence: 99%

“…As a result, tau siRNA-loaded PS 80-coated PLGA NPs significantly suppressed tau expression in cultured primary neural cells. Additionally, they achieved efficient tau silencing in TBI mice with no systemic toxicity when administered during the early or late injury period [142]. PS 80-coated PLGA NPs were developed for the efficient transport of small interfering RNA (siRNA) across the BBB in traumatic brain injury (TBI) [142] (Figure 10).…”

Section: Ps-coated Nps For Efficient Bbb Transportmentioning

confidence: 99%

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Polysorbate-Based Drug Formulations for Brain-Targeted Drug Delivery and Anticancer Therapy

et al. 2021

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Polysorbates (PSs) are synthetic nonionic surfactants consisting of polyethoxy sorbitan fatty acid esters. PSs have been widely employed as emulsifiers and stabilizers in various drug formulations and food additives. Recently, various PS-based formulations have been developed for safe and efficient drug delivery. This review introduces the general features of PSs and PS-based drug carriers, summarizes recent progress in the development of PS-based drug formulations, and discusses the physicochemical properties, biological safety, P-glycoprotein inhibitory properties, and therapeutic applications of PS-based drug formulations. Additionally, recent advances in brain-targeted drug delivery using PS-based drug formulations have been highlighted. This review will help researchers understand the potential of PSs as effective drug formulation agents.

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Section: Ps-coated Nps For Efficient Bbb Transportmentioning

confidence: 99%

Section: Ps-coated Nps For Efficient Bbb Transportmentioning

confidence: 99%

Polysorbate-Based Drug Formulations for Brain-Targeted Drug Delivery and Anticancer Therapy

et al. 2021

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“…Thus they never reach the CNS in significant amounts to have a biological outcome, and this may lead to poor efficacy in a clinical setting. Some examples exist for the entry of free siRNA ( Xie et al, 2020 ) or siRNA-encapsulated nanoparticles ( Li et al, 2021 ) to enter the CNS, however, to date these intriguing approaches are only described to exert their therapeutic effect after a prior breach of the BBB and do not directly show transcytosis of the intact BBB. For example, some studies on traumatic brain injury indicate that BBB may be breached for several days after induction of trauma ( Li et al, 2021 ), others indicate the BBB is permeable for weeks after initial injury (e.g., ischemia, blunt force trauma) ( Strbian et al, 2008 ; Price et al, 2016 ), and some BBB tight junction components can be downregulated for up to 8 weeks ( Nag et al, 2007 ).…”

Section: Discussionmentioning

confidence: 99%

“…Some examples exist for the entry of free siRNA ( Xie et al, 2020 ) or siRNA-encapsulated nanoparticles ( Li et al, 2021 ) to enter the CNS, however, to date these intriguing approaches are only described to exert their therapeutic effect after a prior breach of the BBB and do not directly show transcytosis of the intact BBB. For example, some studies on traumatic brain injury indicate that BBB may be breached for several days after induction of trauma ( Li et al, 2021 ), others indicate the BBB is permeable for weeks after initial injury (e.g., ischemia, blunt force trauma) ( Strbian et al, 2008 ; Price et al, 2016 ), and some BBB tight junction components can be downregulated for up to 8 weeks ( Nag et al, 2007 ). In addition, observation of brain penetration in Alzheimer’s disease and Multiple Sclerosis models have shown a prior breach in the BBB as part of the pathogenesis of the disease ( Ujiie et al, 2003 ; Bennett et al, 2010 ; Biron et al, 2011 ; Biron et al, 2013 ), and siRNA studies in these models similarly cannot be used to conclude transcytosis of siRNA across an intact BBB ( Zhou et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

A Nanomule Peptide Carrier Delivers siRNA Across the Intact Blood-Brain Barrier to Attenuate Ischemic Stroke

Eyford

Singh

Abraham

et al. 2021

Front. Mol. Biosci.

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The blood-brain barrier (BBB) hinders the distribution of therapeutics intended for treatment of neuroinflammation (NI) of the central nervous system. A twelve-amino acid peptide that transcytoses the BBB, termed MTfp, was chemically conjugated to siRNA to create a novel peptide-oligonucleotide conjugate (POC), directed to downregulate NOX4, a gene thought responsible for oxidative stress in ischemic stroke. The MTfp-NOX4 POC has the ability to cross the intact BBB and knockdown NOX4 expression in the brain. Following induction of ischemic stroke, animals pretreated with the POC exhibited significantly smaller infarcts; accompanied by increased protection against neurological deterioration and improved recovery. The data demonstrates that the MTfp can act as a nanomule to facilitate BBB transcytosis of siRNAs; where the NOX-4 specific siRNA moiety can elicit effective therapeutic knockdown of a gene responsible for oxidative stress in the central nervous system. This study is the first to conclusively demonstrate both siRNA-carrier delivery and therapeutic efficacy in any CNS disease model where the BBB remains intact and thus offers new avenues for potential treatments of oxidative stress underlying neuroinflammation in a variety of neuropathologies that are currently refractory to existing therapies.

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“…[ 49 , 50 , 51 , 52 , 53 ] Furthermore, the effect of siRNAs in neurological disorders has been studied to effectively inhibit targeted gene expression in the central nervous system by specific gene silencing. [ 54 , 55 ] Additionally, GalNAc‐siRNA conjugates are exploited for efficient siRNA delivery to liver hepatocytes, inducing targeted gene silencing while guaranteeing the duration of the effect. [ 56 ] Lastly, the suitability of siRNA‐therapeutics in cardiovascular diseases has also been proved.…”

Section: Classification Of Rna Therapeuticsmentioning

confidence: 99%

Nanotechnology‐Assisted RNA Delivery: From Nucleic Acid Therapeutics to COVID‐19 Vaccines

et al. 2021

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In recent years, the main quest of science has been the pioneering of the groundbreaking biomedical strategies needed for achieving a personalized medicine. Ribonucleic acids (RNAs) are outstanding bioactive macromolecules identified as pivotal actors in regulating a wide range of biochemical pathways. The ability to intimately control the cell fate and tissue activities makes RNA‐based drugs the most fascinating family of bioactive agents. However, achieving a widespread application of RNA therapeutics in humans is still a challenging feat, due to both the instability of naked RNA and the presence of biological barriers aimed at hindering the entrance of RNA into cells. Recently, material scientists’ enormous efforts have led to the development of various classes of nanostructured carriers customized to overcome these limitations. This work systematically reviews the current advances in developing the next generation of drugs based on nanotechnology‐assisted RNA delivery. The features of the most used RNA molecules are presented, together with the development strategies and properties of nanostructured vehicles. Also provided is an in‐depth overview of various therapeutic applications of the presented systems, including coronavirus disease vaccines and the newest trends in the field. Lastly, emerging challenges and future perspectives for nanotechnology‐mediated RNA therapies are discussed.

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BBB pathophysiology independent delivery of siRNA in traumatic brain injury

Cited by 8 publications

References 53 publications

Polysorbate-Based Drug Formulations for Brain-Targeted Drug Delivery and Anticancer Therapy

Polysorbate-Based Drug Formulations for Brain-Targeted Drug Delivery and Anticancer Therapy

A Nanomule Peptide Carrier Delivers siRNA Across the Intact Blood-Brain Barrier to Attenuate Ischemic Stroke

Nanotechnology‐Assisted RNA Delivery: From Nucleic Acid Therapeutics to COVID‐19 Vaccines

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