Targeting V600EB-Raf and Akt3 Using Nanoliposomal-Small Interfering RNA Inhibits Cutaneous Melanocytic Lesion Development

Tran, Melissa; Gowda, Raghavendra; Sharma, Arti; Park, Eun Joo; Adair, James H.; Kester, Mark; Smith, Nadine Barrie; Robertson, Gavin P.

doi:10.1158/0008-5472.can-07-6614

Cited by 154 publications

(159 citation statements)

References 42 publications

(72 reference statements)

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“…Historically, researchers have relied on physicochemical methods to facilitate epidermal penetration and cellular delivery of negatively charged nucleic acids (11,(30)(31)(32)(33). However, these methods require high concentrations of free siRNAs, can have unacceptable toxicity in in vivo models, and are limited by the instability of conventional siRNAs.…”

Section: Discussionmentioning

confidence: 99%

“…Although the small treated areas showed a marked reduction in skin thickening, the pain and the impracticality associated with these injections made the approach untenable. Other mechanical approaches, such as ultrasound and laser, have been used to facilitate penetration through the mouse stratum corneum and drive siRNA into skin, but require specialized equipment (30,31,33), limit the area of delivery, and can potentially harm the skin. Recent investigations have demonstrated uptake of siRNAs and DNAs into the epidermis in mice with no stratum corneum (e.g., open wounds or mucosae) or with atopic dermatitis, an inflammatory skin disorder with an ineffective epidermal barrier (33,34).…”

Section: Discussionmentioning

confidence: 99%

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Topical delivery of siRNA-based spherical nucleic acid nanoparticle conjugates for gene regulation

Zheng

Giljohann

Chen

et al. 2012

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

356

288

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Topical application of nucleic acids offers many potential therapeutic advantages for suppressing genes in the skin, and potentially for systemic gene delivery. However, the epidermal barrier typically precludes entry of gene-suppressing therapy unless the barrier is disrupted. We now show that spherical nucleic acid nanoparticle conjugates (SNA-NCs), gold cores surrounded by a dense shell of highly oriented, covalently immobilized siRNA, freely penetrate almost 100% of keratinocytes in vitro, mouse skin, and human epidermis within hours after application. Significantly, these structures can be delivered in a commercial moisturizer or phosphate-buffered saline, and do not require barrier disruption or transfection agents, such as liposomes, peptides, or viruses. SNANCs targeting epidermal growth factor receptor (EGFR), an important gene for epidermal homeostasis, are >100-fold more potent and suppress longer than siRNA delivered with commercial lipid agents in cultured keratinocytes. Topical delivery of 1.5 uM EGFR siRNA (50 nM SNA-NCs) for 3 wk to hairless mouse skin almost completely abolishes EGFR expression, suppresses downstream ERK phosphorylation, and reduces epidermal thickness by almost 40%. Similarly, EGFR mRNA in human skin equivalents is reduced by 52% after 60 h of treatment with 25 nM EGFR SNA-NCs. Treated skin shows no clinical or histological evidence of toxicity. No cytokine activation in mouse blood or tissue samples is observed, and after 3 wk of topical skin treatment, the SNA structures are virtually undetectable in internal organs. SNA conjugates may be promising agents for personalized, topically delivered gene therapy of cutaneous tumors, skin inflammation, and dominant negative genetic skin disorders.T he recent development of small molecule inhibitors and antibodies that target components of signaling pathways has revolutionized the treatment of cancers, inflammatory diseases, and genetic disorders, including those that largely manifest in skin (1-3). These protein-based therapeutics, however, are costly, have limited targeting ability, and, when delivered through traditional intravenous or gastrointestinal routes, can lead to systemic toxicity (4, 5). Topical delivery is particularly attractive for the therapy of skin disorders. However, proteins larger than a few hundred daltons cannot easily enter the skin, and high concentrations of proteins must be applied for a cutaneous effect (6). An alternative to protein-based pathway inhibition involves the blocking and/or degradation of precursor mRNA before translation into protein. Gene silencing leads to down-regulation of protein expression and functions with greater specificity than inhibitors of protein function (7). In fact, targeted gene suppression by antisense DNA and siRNA has shown promising preclinical results, and/or is currently in clinical trials for a variety of diseases, including many forms of cancer (e.g., melanoma, neuroblastoma, and pancreatic adenocarcinoma), genetic disorders, and macular degeneration (8). For gene su...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Topical delivery of siRNA-based spherical nucleic acid nanoparticle conjugates for gene regulation

Zheng

Giljohann

Chen

et al. 2012

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

356

288

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“…Other studies have shown that PI3K and MEK inhibitors synergise to reduce growth and survival of melanoma cell lines grown under 3D organotypic cell culture conditions Meier et al, 2007). There is also evidence that siRNA knockdown of AKT3 and BRAF V600E leads to the enhanced inhibition of melanoma xenograft growth in nude mice Tran et al, 2008). …”

Section: Suitable Combination Targets: the Pi3k Pathway?mentioning

confidence: 97%

Integrating BRAF/MEK inhibitors into combination therapy for melanoma

Smalley

Flaherty

2009

Br J Cancer

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“…Furthermore, the increase in Akt3 activity in their melanoma model was associated with both Akt3 gene amplification and mutations in PTEN (104). Subsequently, data from the Robertson group (42,105) demonstrated a direct link between tumor progression in melanoma cells with Akt3-dependent phosphorylation of B-RAF.…”

Section: Akt3 and Melanomamentioning

confidence: 98%

The Akt isoforms, their unique functions and potential as anticancer therapeutic targets

Santi¹,

Douglas²,

Lee³

2010

BioMolecular Concepts

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Akt (also known as protein kinase B or PKB) is the major downstream nodal point of the PI3K signaling pathway. This pathway is a promising anticancer therapeutic target, because constitutive activation of the PI3K-Akt pathway is correlated with tumor development, progression, poor prognosis, and resistance to cancer therapies. The Akt serine/threonine kinase regulates diverse cellular functions including cell growth, proliferation, glucose metabolism, and survival. Although all three known Akt isoforms (Akt1-3) are encoded by separate genes, their amino acid sequences show a high degree of similarity. For this and other reasons, it has long been assumed that all three Akt isoforms are activated in the same way, and their functions largely overlap. However, accumulating lines of evidence now suggest that the three Akt isoforms might have unique modes of activation and many distinct functions. In particular, it has recently been found that the Akt isoforms are localized at different subcellular compartments in both adipocytes and cancer cells. In this review, we highlight the unique roles of each Akt isoform by introducing published data obtained from both in vitro and in vivo studies. We also discuss the significant potential of the Akt isoforms as effective anticancer therapeutic targets.

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Targeting V600EB-Raf and Akt3 Using Nanoliposomal-Small Interfering RNA Inhibits Cutaneous Melanocytic Lesion Development

Cited by 154 publications

References 42 publications

Topical delivery of siRNA-based spherical nucleic acid nanoparticle conjugates for gene regulation

Topical delivery of siRNA-based spherical nucleic acid nanoparticle conjugates for gene regulation

Integrating BRAF/MEK inhibitors into combination therapy for melanoma

The Akt isoforms, their unique functions and potential as anticancer therapeutic targets

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