<i>β</i>-Galactosidase Gene Transfer to Human Malignant Glioma <i>In Vivo</i> Using Replication-Deficient Retroviruses and Adenoviruses

Puumalainen, Anu-Maaria; Vapalahti, Matti; Agrawal, Reitu; Kossila, Maija; Laukkanen, Johanna; Lehtolainen, Pauliina; Viita, Helena; Paljärvi, Leo; Vanninen, Ritva; Ylä‐Herttuala, Seppo

doi:10.1089/hum.1998.9.12-1769

Cited by 178 publications

(123 citation statements)

References 18 publications

Supporting

Mentioning

118

Contrasting

Unclassified

Order By: Relevance

“…In parallel to what is seen in clinical trials featuring intratumoral administration, direct injection resulted in patchy infection of mostly the needle tract. 18 The implant had resorbed completely by day 21. Next, virus release was studied in orthotopic murine tumors, which may be superior over subcutaneous models, as they capture the effect of the tumor environment better.…”

Section: Silicated Adenovirus L Kangasniemi Et Almentioning

confidence: 98%

Extended release of adenovirus from silica implants in vitro and in vivo

et al. 2008

View full text Add to dashboard Cite

Despite promising preclinical results, the clinical benefits of cancer gene therapy have been modest heretofore. The main obstacle continues to be the level and persistence of gene delivery to sufficiently large areas of the tumor. One approach for overcoming this might entail extended local virus release. We studied the utility of silica gel monoliths for delivery of adenovirus to advanced orthotopic gastric and pancreatic cancer tumors. Initially, the biochemical properties of the silica-virus matrix were studied and nearly linear release as a function of time was detected. Virus stayed infective for weeks at +37 1C and months at +4 1C, which may facilitate storage and distribution. In vivo, extended release of functional replication deficient and also replication-competent, capsid-modified oncolytic viruses was seen. Treatment of mice with pancreatic cancer doubled their survival ( Po0.001). Also, silica gel-based delivery slowed the development of antiadenovirus antibodies.

show abstract

Section: Silicated Adenovirus L Kangasniemi Et Almentioning

confidence: 98%

Extended release of adenovirus from silica implants in vitro and in vivo

et al. 2008

View full text Add to dashboard Cite

show abstract

“…Adenoviruses were analyzed to be free from helper viruses, lipopolysaccharides and bacteriological contaminants. 33,34 Animal model Balb/cA-nu female nude mice (n ¼ 42), 8-10-weeks old, were used for the studies. Ovarian carcinoma was produced by inoculating 1 Â 10 7 SKOV-3m cells into the peritoneal cavity of the nude mice with a 22 G needle.…”

Section: Viral Vectorsmentioning

confidence: 99%

Cotargeting of VEGFR-1 and -3 and angiopoietin receptor Tie2 reduces the growth of solid human ovarian cancer in mice

et al. 2010

View full text Add to dashboard Cite

Despite optimal surgery and chemotherapy, the prognosis of ovarian cancer patients remains poor and new treatments are urgently needed. Solid tumors require the formation of new vessels for growth and metastasis. In the present study, we have used soluble vascular endothelial growth factor (sVEGF) receptors sVEGFR-1 and -3, soluble receptors Tie1 and Tie2 and their combinations in an ovarian cancer xenograft model. Human ovarian cancer cells were injected intraperitoneally into nude mice (n ¼ 42) and magnetic resonance imaging (MRI) was used for confirming tumors before gene delivery. Treatment with combined AdsVEGFR-1, AdsVEGFR-3 and AdsTie2 significantly decreased the size of the intraperitoneal tumors compared with the controls (AdLacZ; P ¼ 0.038) with significantly less microvessels and vascular area. Unexpectedly, treatment with combined AdsTie1 and AdsTie2 led to a dramatic shortening of the survival which was not observed in the groups receiving either of the soluble receptors alone (P ¼ 0.031). The only difference to other treatments was liver toxicity observed after the combined Tie receptor treatment.In conclusion, combined inhibition of VEGFR-1, VEGFR-3 and Tie2 pathways was safe and provided efficient therapy for ovarian cancer in mice.

show abstract

“…2,9,11 As short-term side effects, they have caused transient inflammatory effects, such as short-term fever, elevation of C-reactive protein (CRP) and formation of anti-adenovirus antibodies. 2,12,13 Liposomes are safe, but their gene transfer efficiency is much lower when compared with that of adenoviruses. The therapeutic effect of non-viral gene transfer is long lasting compared with that of adenoviral gene transfer.…”

Section: Introductionmentioning

confidence: 99%