Biodistribution of Radiolabeled Lipid–DNA Complexes and DNA in Mice

Niven, Ralph W.; Pearlman, Rodney; Wedeking, Todd; MacKeigan, Jeffrey P.; Noker, Patricia E.; Simpson-Herren, Linda; Smith, Jai

doi:10.1021/js980087a

Cited by 103 publications

(65 citation statements)

References 16 publications

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“…It has been reported that incubation in pure serum or serum-containing media could decrease the extent of lipoplex delivery and alter its intracellular fate 19,20) and even cause the lipoplex to disintegrate upon prolonged exposure. 18,21) However, an injected lipoplex is rapidly cleared from the circulation 18,22) and internalized in the lungs, 23) thus ruling out long-term exposure to serum. In addition, Sakurai et al showed the pre-incubation of a DOTAP/Chol lipoplex with serum for as long as 30 min did not significantly impair lipofection in the lungs.…”

Section: Discussionmentioning

confidence: 99%

“…5). The first pass entrapment (60-80% of the liposomes are entrapped within minutes after intravenous injection) 18,22,28) can be attributed to the highly extended lung capillary bed and was proposed to explain the predominant gene expression in the lungs. 28,29) Ito et al 30) recently reported that vascular endothelial cells, probably under angiogenesis, in the lungs of tumor bearing mice, which demonstrates an increased uptake of cationic liposome-DNA complexes and transgene expression compared to normal mice.…”

Section: Discussionmentioning

confidence: 99%

“…The morbidity rate of lung cancer has been rising particularly rapidly, and a pressing countermeasure is necessary. 16) Lipoplexes usually accumulate largely in the lung, although the distribution changes with time: lipoplexes are found in the lung shortly after intravenous injection but eventually accumulate in the liver after 24 or 48 h. 17,18) This is because the lipoplex form aggregates in the blood stream, and is captured in the first capillary en-countered. If the pDNA could be quickly transferred from lipoplexes to pulmonary endothelial cells after being captured in a capillary of the lung, an enhanced transgene expression might be obtained.…”

mentioning

confidence: 99%

See 2 more Smart Citations

Increased Gene Expression by Cationic Liposomes (TFL-3) in Lung Metastases Following Intravenous Injection

Ishida

Okada

et al. 2005

Biological & Pharmaceutical Bulletin

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

Increased Gene Expression by Cationic Liposomes (TFL-3) in Lung Metastases Following Intravenous Injection

Ishida

Okada

et al. 2005

Biological & Pharmaceutical Bulletin

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“…It was interesting to find that both chitosan and chitosan oligosaccharide can not only influence the particle shape and morphology but enhance the dispersibility of spray-dried powders. Chitosan oligosaccharide, possessing the properties of soluble, biodegradable, biocompatible, bioadhesive and nontoxic, 38) has the ability to enhance mucosal absorption by opening tight junctions, 39) potentially resulting in an increase of drug absorption subsequent to inhalation. In our study, the addition of chitosan oligosaccharide in formulations can achieve higher spray-dried yields (Figs.…”

Section: Resultsmentioning

confidence: 99%

Optimization and Characterization of Dry Powder of Fanhuncaoin for Inhalation Based on Selection of Excipients

Yang

Wang

Pan

et al. 2011

CHEMICAL & PHARMACEUTICAL BULLETIN

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Regular ArticleDrug delivery to the lungs is highly desirable, especially in patients with specific pulmonary diseases such as chronic pulmonary infections. It can reduce systemic side effects and increase doses of the applicable medication at the site of drug action. It's also a good idea to choose inhalation for systemic therapies because the respiratory region of the lung has an enormous surface area (80-100 m 2 /adult), a highly permeable membrane (0.1-0.2 mm) for the absorption of medication into the blood and a blood flow about 5 l/min, which rapidly transports molecules throughout the body. 1) Large protein molecules, which degrade in the terrible gastrointestinal conditions, can be delivered via the pulmonary route. In addition, it is a needle-free delivery system capable of increasing the compliance of patients.The 1-5 mm aerodynamic diameter range is needed for particles to be inhaled in order to avoid deposition in the oropharynx and maximize deposition in the lower respiratory tract.2) Generally, drugs for inhalation in dry powder inhaler (DPI) systems are micronized to achieve the requisite size; however, particles in this size range show strong interparticulate cohesion, leading to poor powder flow properties.3,4) In addition, factors that are known to influence the aerosolization properties of dry powders, such as particle morphology, density and surface composition, can not be well controlled by the micronization process. 5)Spray drying, an alternative approach to the generation of potentially respirable powders with respect to local pulmonary drug delivery, offers advantages to manipulate and control a variety of parameters such as temperature and relative humidity, solute concentration, solvent composition, solution and gas feed rate, droplet size, etc. This allows optimization of particle characteristics such as particle size, size distribution, density and morphology, and then macroscopic powder properties such as bulk density, flowability and dispersibility. 6)Senecio cannabifolius LESS. (Kuan Ye Fan Hun Cao in Chinese), as one species of Senecio genus of Compositae family, shows the effects on dispelling ecchymoma, anastalsis and algesic. As one kind of folk medicine, it's usually used to treat the diseases, such as virus influenza and many kinds of inflammatories. Unfortunately, In 2004, the importing of many kinds of preparations made from the species of Senecio genus from China had been prohibited by American and Europe drug administrative departments, because of the existence of one of its chemical constituents named pyrrolizidine alkaloids, which exhibited the chronical hepatotoxicity (liver toxicity) and cancerigenic possibility to the human beings. In order to deal with the contradiction between the toxicity and efficiency on the treatment, 52 compounds were obtained from the herb by many kinds of isolation method, such as silica gel chromatography, Lobar column, semi-preparative HPLC (PHPLC) and so on. Among the 52 compounds, 14 of them were isolated from the Senecio genus for the f...

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“…Since free oligonucleotides and DNA are rapidly degraded by serum nucleases, 4) many efforts are focused on developing the carriers to protect and deliver these materials into targeted cells. Two delivery systems namely viral and non-viral vectors are currently developed to solve the problems.…”

mentioning

confidence: 99%

Synergistic Effect of Cationic Lipids with Different Polarheads, Central Core Structures and Hydrophobic Tails on Gene Transfection Efficiency

Niyomtham

Apiratikul

Chanchang

et al. 2014

Biological & Pharmaceutical Bulletin

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Lipid-mediated delivery of DNA into cells holds great promise both for gene therapy and basic research applications. The primary approach to improving transfection efficiency is the design and synthesis of novel cationic lipids. Alternatively, using the synergistic effect of different cationic mixtures can provide another approach to increasing transfection efficiency. This paper describes the synergistic effect of lipids with different polarheads, central core structures and hydrophobic tails. The enhancement of cellular transfection into HEK293 cells was observed by combining two lipids having aminoglycerol and di(hydroxylethyl)amino core structures at a 1 : 1 weight ratio. Additionally, the liposome formation of these lipids with the helper lipid, 1,2-dioleoyl-propyl-3-phosphatidylethanolamine (DOPE), at the weight ratio of 1 : 1 can provide higher transfection efficiency into HEK293, MCF-7 and HeLa cells than Lipofectamine™ 2000. Our finding indicated that cationic liposomes comprised of a mixture of lipids with different polarheads, central core structures and hydrophobic tails should be very promising in liposome-mediated gene delivery in vitro and in vivo.Key words cationic liposome; synergistic effect; DNA delivery; non-viral vector.Gene therapy has gained significant attention over past two decades as an alternative method to treat genetic disorders 1,2) as well as cancers.3) One fundamental of gene therapy is the delivery system that can introduce and stabilize genetic material. Since free oligonucleotides and DNA are rapidly degraded by serum nucleases, 4) many efforts are focused on developing the carriers to protect and deliver these materials into targeted cells. Two delivery systems namely viral and non-viral vectors are currently developed to solve the problems. Viral carriers have known to be one of the most effective gene delivery methods for in vivo application. [5][6][7][8] Over one thousand gene therapy clinical trials have been completed or approved; two-thirds of which performed by viral vectors. 8)However, the limitation of viral vectors concerning toxicity, immunogenicity, scale-up procedures and their relatively small capacity for therapeutic DNA has prompted the development non-viral vectors. Delivery systems based on non-viral vectors, for example cationic lipids, dendrimers or cationic polymers, have been the focus of much recent research.9) Non-viral systems have proved to be generally less toxic or immunogenic, more easily to produce and a greater stability.Cationic liposomes are one of the most extensively studied of non-viral vectors because of their lesser immunogenic nature, ease of production and handle, and ability to deliver large pieces of DNA. Cationic liposomes, like other non-viral vectors bearing positive charge, interact with the negatively charged phosphate backbone of nucleic acids to form a compact structure and facilitate cellular uptake by endocytic routes. [10][11][12][13] Since the first application of cationic lipid in DNA delivery, 14) numerous cationic lipids...

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Biodistribution of Radiolabeled Lipid–DNA Complexes and DNA in Mice

Cited by 103 publications

References 16 publications

Increased Gene Expression by Cationic Liposomes (TFL-3) in Lung Metastases Following Intravenous Injection

Increased Gene Expression by Cationic Liposomes (TFL-3) in Lung Metastases Following Intravenous Injection

Optimization and Characterization of Dry Powder of Fanhuncaoin for Inhalation Based on Selection of Excipients

Synergistic Effect of Cationic Lipids with Different Polarheads, Central Core Structures and Hydrophobic Tails on Gene Transfection Efficiency

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