Keren Ofir scite author profile

In a model of growth-restricted sheep pregnancy, it was previously demonstrated that transient uterine artery VEGF overexpression can improve fetal growth. This approach was tested in guinea-pig pregnancies, where placental physiology is more similar to humans. Fetal growth restriction (FGR) was attained through peri-conceptual nutrient restriction in virgin guinea pigs. Ad.VEGF-A or Ad.LacZ (1 × 10vp) was applied at mid-gestation via laparotomy, delivered externally to the uterine circulation with thermosensitive gel. At short-term (3-8 days post surgery) or at term gestation, pups were weighed, and tissues were sampled for vector spread analysis, VEGF expression, and its downstream effects. Fetal weight at term was increased (88.01 ± 13.36 g; n = 26) in Ad.VEGF-A-treated animals compared with Ad.LacZ-treated animals (85.52 ± 13.00 g; n = 19; p = 0.028). The brain, liver, and lung weight and crown rump length were significantly larger in short-term analyses, as well as VEGF expression in transduced tissues. At term, molecular analyses confirmed the presence of VEGF transgene in target tissues but not in fetal samples. Tissue histology analysis and blood biochemistry/hematological examination were comparable with controls. Uterine artery relaxation in Ad.VEGF-A-treated dams was higher compared with Ad.LacZ-treated dams. Maternal uterine artery Ad.VEGF-A increases fetal growth velocity and term fetal weight in growth-restricted guinea-pig pregnancy.

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Gene Targeting to the Uteroplacental Circulation of Pregnant Guinea Pigs

Mehta

Ofir

Swanson

et al. 2016

Reprod. Sci.

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Our study aimed to target adenoviral gene therapy to the uteroplacental circulation of pregnant guinea pigs in order to develop a novel therapy for fetal growth restriction. Four methods of delivery of an adenovirus encoding β-galactosidase (Ad.LacZ) were evaluated: intravascular injection using phosphate-buffered saline (PBS) into (1) uterine artery (UtA) or (2) internal iliac artery or external administration in (3) PBS or (4) pluronic F-127 gel (Sigma Aldrich). Postmortem examination was performed 4 to 7 days after gene transfer. Tissue transduction was assessed by X-gal histochemistry and enzyme-linked immunosorbent assay. External vascular application of the adenovirus vector in combination with pluronic gel had 91.7% success rate in terms of administration (85% maternal survival) and gave the best results for maternal/fetal survival and local transduction efficiency without any spread to maternal or fetal tissues. This study suggests an optimal method of gene delivery to the UtAs of a small rodent for preclinical studies.

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Keren Ofir

Uterine rupture: risk factors and pregnancy outcome

Uterine rupture: differences between a scarred and an unscarred uterus

Subsequent pregnancy after stillbirth: obstetrical and medical risks

Maternal Therapy with Ad.VEGF-A₁₆₅Increases Fetal Weight at Term in a Guinea-Pig Model of Fetal Growth Restriction

Gene Targeting to the Uteroplacental Circulation of Pregnant Guinea Pigs

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Keren Ofir

Uterine rupture: risk factors and pregnancy outcome

Uterine rupture: differences between a scarred and an unscarred uterus

Subsequent pregnancy after stillbirth: obstetrical and medical risks

Maternal Therapy with Ad.VEGF-A165Increases Fetal Weight at Term in a Guinea-Pig Model of Fetal Growth Restriction

Gene Targeting to the Uteroplacental Circulation of Pregnant Guinea Pigs

Contact Info

Product

Resources

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Maternal Therapy with Ad.VEGF-A₁₆₅Increases Fetal Weight at Term in a Guinea-Pig Model of Fetal Growth Restriction