In vivo endothelial siRNA delivery using polymeric nanoparticles with low molecular weight

Dahlman, James E.; Barnes, Carmen; Khan, Omar F.; Thiriot, Aude; Jhunjunwala, Siddharth; Shaw, Taylor E.; Xing, Yiping; Sager, Hendrik B.; Sahay, Gaurav; Speciner, Lauren; Báder, A.; Bogorad, Roman L.; Yin, Hao; Racie, Tim; Dong, Yizhou; Jiang, Shan; Seedorf, Danielle; Dave, Apeksha; Sandhu, Kamaljeet Singh; Webber, Matthew J.; Novobrantseva, Tatiana; Ruda, Vera M.; Lytton-Jean, Abigail K. R.; Levins, Christopher G.; Kalish, Brian T.; Mudge, Dayna K.; Pérez, Mario J.; Abezgauz, Ludmila; Dutta, Partha; Smith, Lynelle P.; Charissé, Klaus; Kieran, Mark W.; Fitzgerald, Kevin; Nahrendorf, Matthias; Danino, Dganit; Tuder, Rubin M.; Andrian, Ulrich H. von; Akinc, Akin; Panigrahy, Dipak; Schroeder, Avi; Koteliansky, Victor; Langer, Robert; Anderson, Daniel G.

doi:10.1038/nnano.2014.84

Cited by 477 publications

(464 citation statements)

References 35 publications

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“…Instead of using transfection reagents, LPNPs serve as the packaging and delivery vehicle by shielding the negative charge of the siRNA duplex while offering the benefits of low toxicity and decreased liver targeting and kidney clearance when given systemically in the blood stream (23). To examine the feasibility of using LPNPs to deliver RNAi to BTICs and potentially to a tumor-associated microenvironment such as tumor-associated blood vessels, in vitro knockdown of the four master TF mRNAs was performed using 7C1 LPNPs formulated with a combination of siRNAs.…”

Section: Tf Profiling and Selection Of Tumor Cell Lines For Therapeutmentioning

confidence: 99%

“…conjugating epoxide-terminated lipids to low-molecular-weight polyamines with an epoxide ring-opening reaction (23). The resultant nano constructs then were evaluated for their ability to complex with siRNA and knock down gene expression in vitro.…”

mentioning

confidence: 99%

“…The most effective candidates were selected after in vivo assessment. One compound, named "7C1," was identified from a library of more than 500 candidate delivery materials as the most effective in silencing target genes in vasculature, with a higher performance per dose ratio than previously reported siRNA nano delivery vehicles (15,23). The capacity to multitarget and the ease of synthesis make 7C1 an attractive therapeutic vehicle for antitumor RNAi.…”

mentioning

confidence: 99%

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Multiplexed RNAi therapy against brain tumor-initiating cells via lipopolymeric nanoparticle infusion delays glioblastoma progression

Khan

Suvà

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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104

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Brain tumor-initiating cells (BTICs) have been identified as key contributors to therapy resistance, recurrence, and progression of diffuse gliomas, particularly glioblastoma (GBM). BTICs are elusive therapeutic targets that reside across the blood-brain barrier, underscoring the urgent need to develop novel therapeutic strategies. Additionally, intratumoral heterogeneity and adaptations to therapeutic pressure by BTICs impede the discovery of effective anti-BTIC therapies and limit the efficacy of individual gene targeting. Recent discoveries in the genetic and epigenetic determinants of BTIC tumorigenesis offer novel opportunities for RNAi-mediated targeting of BTICs. Here we show that BTIC growth arrest in vitro and in vivo is accomplished via concurrent siRNA knockdown of four transcription factors (SOX2, OLIG2, SALL2, and POU3F2) that drive the proneural BTIC phenotype delivered by multiplexed siRNA encapsulation in the lipopolymeric nanoparticle 7C1. Importantly, we demonstrate that 7C1 nano-encapsulation of multiplexed RNAi is a viable BTICtargeting strategy when delivered directly in vivo in an established mouse brain tumor. Therapeutic potential was most evident via a convection-enhanced delivery method, which shows significant extension of median survival in two patient-derived BTIC xenograft mouse models of GBM. Our study suggests that there is potential advantage in multiplexed targeting strategies for BTICs and establishes a flexible nonviral gene therapy platform with the capacity to channel multiplexed RNAi schemes to address the challenges posed by tumor heterogeneity.siRNA | lipopolymeric nanoparticle | glioblastoma transcription factor | brain tumor-initiating cells | convection-enhanced delivery G lioblastoma (GBM) is one of the most challenging tumors to treat (1, 2). Despite decades of research and maximal clinical combination therapy encompassing surgical resection, chemotherapy, and radiation, the median life expectancy of patients has not been extended beyond 2 y after diagnosis (2). Increasing evidence suggests that the genetic, epigenetic, and signaling heterogeneity of GBM underlies the ineffectiveness of currently available therapeutics (1, 2). Additionally, therapeutic schemes devised to challenge brain tumor cells are frequently thwarted by insufficient delivery caused by pharmacokinetics, the blood-brain barrier (BBB), and an altered tumor microenvironment in which tumor-derived signaling recruits immunomodulatory cells and induces extracellular matrix remodeling to build safe harbors of tumorigenic niches (3-5). These obstacles call for tailored therapeutic strategies to counter tumor heterogeneity and overcome roadblocks in delivery. RNAi targeting drivers of tumorigenesis shows strong potential to supplement the development of traditional small-molecule pharmaceutics (6). However, delivery remains a key obstacle for efficient RNAi against tumor drivers (5,7,8). RNA-sequencing analysis of patient tissue combined with histology and in situ hybridization (Ivy Glioblastoma Atlas Pro...

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Section: Tf Profiling and Selection Of Tumor Cell Lines For Therapeutmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Multiplexed RNAi therapy against brain tumor-initiating cells via lipopolymeric nanoparticle infusion delays glioblastoma progression

Khan

Suvà

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

104

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“…Preferential targeting of the pulmonary endothelium rather than the systemic endothelium has been demonstrated and promoted using different nanoparticle-based oligonucleotide delivery partners (86). Multiple strategies for proprietary modifications of the nucleotide backbone provide resistance to degradation in vivo, and provide the means to improve stability and efficacy.…”

Section: Therapeutic Potential Of Mirna In Pulmonary Vascular Diseasementioning

confidence: 99%

Translational Advances in the Field of Pulmonary Hypertension.Translating MicroRNA Biology in Pulmonary Hypertension. It Will Take More Than “miR” Words

Chun

Bonnet²,

Chan

2017

Am J Respir Crit Care Med

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“…Approaches like those discussed above are not only be useful for DNA delivery, but for new methods of gene therapy such as RNAi (RNA interference) as well. In particular with Dan Anderson, we have created libraries of thousands of lipids and they are being used as delivery systems for RNAi (Akinc et al 2008;Dahlman et al 2014).…”

Section: Expanding Our Early Findings and Creating New Biomaterialsmentioning

confidence: 99%

Chemical materials and their regulation of the movement of molecules

Langer

2015

Quart. Rev. Biophys.

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Abstract. Materials chemistry has been fundamental to the enormous field that encompasses the delivery of molecules both to desired sites and/or at desired rates and durations. The field encompasses the delivery of molecules including fertilizers, pesticides, herbicides, food ingredients, fragrances and biopharmaceuticals. A personal perspective is provided on our early work in this field that has enabled the controlled release of ionic substances and macromolecules. Also discussed are new paradigms in creating biomaterials for human use, the non-invasive delivery of molecules through the skin and lungs, the development of intelligent delivery systems and extensions to nanomedicine. With the advent of potentially newer biopharmaceutics such as siRNA, mRNA and gene editing approaches and their use being limited by delivery, future research in this field may be more critical than ever before.

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In vivo endothelial siRNA delivery using polymeric nanoparticles with low molecular weight

Cited by 477 publications

References 35 publications

Multiplexed RNAi therapy against brain tumor-initiating cells via lipopolymeric nanoparticle infusion delays glioblastoma progression

Multiplexed RNAi therapy against brain tumor-initiating cells via lipopolymeric nanoparticle infusion delays glioblastoma progression

Translational Advances in the Field of Pulmonary Hypertension.Translating MicroRNA Biology in Pulmonary Hypertension. It Will Take More Than “miR” Words

Chemical materials and their regulation of the movement of molecules

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