Leptin gene therapy and daily protein administration: a comparative study in the ob/ob mouse

Morsy, Manal; Gu, Mingcheng; Zhao, Jun; Holder, Daniel; Rogers, Imogen; Pouch, W J; Motzel, Sherri L.; Klein, Hilton J.; Gupta, Sanchita; Xie, Liyang; Tota, Michael R.; Rosenblum, Charles; Caskey, C. Thomas

doi:10.1038/sj.gt.3300565

Cited by 41 publications

(37 citation statements)

References 8 publications

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“…Construction of Ad-leptin and Ad-␤-galalactosidase (␤-gal) recombinant vectors has been described (30). The expression cassettes contain the human cytomegalovirus (HCMV) promoter (Invitrogen), the transgene, and the bovine growth hormone poly(A) sequence.…”

Section: Construction Of Vectorsmentioning

confidence: 99%

“…For Northern blot analysis, total RNA was extracted (Trizol, GIBCO) from livers of Ad-leptin-treated and HD-leptin-treated mice at 1-, 2-, 4-, and 8-week intervals, and untreated mice. Leptin RNA message was detected by Northern blot analysis (35) using leptin cDNA as a probe that recognizes a single Ϸ500 bp band (30). A probe for ␤-actin was used as the internal control (Ϸ1 kb) (Biochain, San Leandro, CA).…”

Section: Construction Of Vectorsmentioning

confidence: 99%

“…Daily delivery of recombinant leptin protein was shown to induce weight reduction, suppress appetite, and decrease blood insulin and glucose levels in ob͞ob (leptindeficient) mice (27)(28)(29). It has been shown that delivery of the leptin cDNA by first-generation Ad vectors (Ad-leptin) may substitute for daily recombinant leptin protein treatment, although the effects were transient in both lean and ob͞ob treated mice (7,30). In the present study, we delivered the leptin cDNA using the HD virus (HD-leptin), testing the hypothesis that elimination of the viral protein coding sequences would diminish the vector's cellular immunogenicity and toxicity, and hence support its longevity in vivo.…”

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confidence: 99%

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An adenoviral vector deleted for all viral coding sequences results in enhanced safety and extended expression of a leptin transgene

Morsy

Motzel

et al. 1998

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

357

237

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Adenoviral (Ad)-mediated in vivo gene transfer and expression are limited in part by cellular immune responses to viral-encoded proteins and͞or transgene immunogenicity. In an attempt to diminish the former responses, we have previously developed and described helper-dependent (HD) Ad vectors in which the viral protein coding sequences are completely eliminated. These HD vectors have up to 37 kb insert capacity, are easily propagated in a Cre recombinasebased system, and can be produced to high concentration and purity (>99.9% helper-free vector). In this study, we compared safety and efficacy of leptin gene delivery mediated by an HD vector (HD-leptin) and a first-generation E1-deleted Ad vector (Ad-leptin) in normal lean and ob͞ob (leptindeficient) mice. In contrast to evidence of liver toxicity, inf lammation, and cellular infiltration observed with Adleptin delivery in mice, HD-leptin delivery was associated with a significant improvement in associated safety͞toxicity and resulted in efficient gene delivery, prolonged elevation of serum leptin levels, and associated weight loss. The greater safety, efficient gene delivery, and increased insert capacity of HD vectors are significant improvements over current Ad vectors and represent favorable features especially for clinical gene therapy applications. Adenoviral (Ad) vectors are currently among the most efficient gene transfer vehicles for both in vitro and in vivo delivery, but the utilization of current Ad vectors for many gene therapy applications is limited by the transient nature of transgene expression obtained by these vectors (1-7). Several factors have been shown to contribute to and modulate the duration of Ad-mediated gene expression and the immunogenicity of these vectors, including ''leaky'' viral protein expression and the transgene that is delivered (8-15). The development of Ad vectors that are deleted in all viral protein-coding sequences offers the prospect of a potentially safer, less immunogenic vector with an insert capacity of up to 37 kb (16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26). This vector is supplied in trans with the structural proteins required for packaging and rescue and is thus helper-dependent (HD) (24).Leptin has been recently identified as a potent modulator of weight and food intake. Daily delivery of recombinant leptin protein was shown to induce weight reduction, suppress appetite, and decrease blood insulin and glucose levels in ob͞ob (leptindeficient) mice (27)(28)(29). It has been shown that delivery of the leptin cDNA by first-generation Ad vectors (Ad-leptin) may substitute for daily recombinant leptin protein treatment, although the effects were transient in both lean and ob͞ob treated mice (7,30). In the present study, we delivered the leptin cDNA using the HD virus (HD-leptin), testing the hypothesis that elimination of the viral protein coding sequences would diminish the vector's cellular immunogenicity and toxicity, and hence support its longevity in vivo. Because both the viral proteins and the trans...

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Section: Construction Of Vectorsmentioning

confidence: 99%

Section: Construction Of Vectorsmentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

An adenoviral vector deleted for all viral coding sequences results in enhanced safety and extended expression of a leptin transgene

Morsy

Motzel

et al. 1998

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

357

237

View full text Add to dashboard Cite

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“…Furthermore, treatment of these animals with a recombinant adenovirus expressing the mouse leptin cDNA (AdRSV-leptin) resulted in a rapid reduction in food consumption and drastic weight loss, which led to a complete, although transient, correction of obesity and diabetes as serum leptin levels decreased after 2-3 weeks (Muzzin et al 1996). Comparing the efficacy of daily injection of recombinant leptin protein with adenovirusmediated delivery of leptin for obesity treatment, Morsy et al (1998b) found that there is a continuous chronic secretion of leptin mediated by gene delivery v. the intermittent bolus delivery and rapid clearance of the daily leptin protein injection. Furthermore, in vivo studies suggest that leptin effects are better achieved at the lower steady-state levels achieved by gene therapy.…”

Section: Gene Transfer Strategies In Obesity Modelsmentioning

confidence: 99%

Methodological approaches to assess body-weight regulation and aetiology of obesity

Martí

Jebb

et al. 2000

Proc. Nutr. Soc.

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Obesity, which is becoming one of the major health hazards in developed and developing societies, results from a long-term positive energy balance. Body-weight regulation and stability depend on an axis with three interrelated components: food intake, energy expenditure and adipogenesis, although there are still many unknown features concerning fuel homeostasis and energy balance. Biochemical processes are interconnected, and a separate consideration of each component is often useful for methodological purposes and to achieve a better understanding of the whole system. Thus, many different experimental approaches can be applied by using laboratory animals, cell culture or human subjects to unravel the molecular mechanisms which participate in body-weight regulation. Thus, both in vitro (cellular and subcellular models) and in vivo methods have dramatically increased our knowledge of weight control. Several strategies in obesity research are reported here, exploiting the opportunities of the molecular era as well as novel whole-body approaches, which will impact on the development of new targets for obesity management and prevention.

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“…1 Leptin gene delivery is substantially more effective in correcting genetic obesity than daily leptin infusion, despite higher peak serum leptin levels with the latter. 2 Peripheral administration of virally encoded leptin requires that the leptin crosses the blood-brain barrier (BBB) to reach its primary hypothalamic targets, but this transport system is saturated at serum leptin levels seen in obese animals. 3 Since several obese, leptin-resistant models respond better to central versus peripheral administration of recombinant leptin, [4][5][6] it has been reasoned that central delivery of the leptin gene would be superior to peripheral delivery.…”

Section: Introductionmentioning

confidence: 99%

Hypothalamic delivery of doxycycline-inducible leptin gene allows for reversible transgene expression and physiological responses

et al. 2002

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Our purpose was to incorporate regulation into the recombinant adeno-associated virus encoding leptin by introducing a tet-inducible promotor. This system, TET-Ob, allows for control of leptin gene expression via doxycycline in drinking water. F344XBN rats (aged 4 months) were given a hypothalamic injection of TET-Ob or control virus. During 34 days of doxycycline (doxy) administration to all rats (STAGE 1), TET-Ob rats gained 50.7% less mass, ate 10.4% less food, and had a 77.5% reduction in serum leptin as compared with controls. Doxy was then withdrawn from half of the TET-Ob rats for 32 days (TET-Ob-OFF), while half continued to receive doxy (TET-Ob-ON) (stage 2). During stage 2, TET-

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Leptin gene therapy and daily protein administration: a comparative study in the ob/ob mouse

Cited by 41 publications

References 8 publications

An adenoviral vector deleted for all viral coding sequences results in enhanced safety and extended expression of a leptin transgene

An adenoviral vector deleted for all viral coding sequences results in enhanced safety and extended expression of a leptin transgene

Methodological approaches to assess body-weight regulation and aetiology of obesity

Hypothalamic delivery of doxycycline-inducible leptin gene allows for reversible transgene expression and physiological responses

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