Antisense inhibition of urokinase: Effect on malignancy in a human osteosarcoma cell line

Expression of urokinase‐type plasminogen activator (u‐PA) strongly correlates with a malignant tumor cell phenotype. In the multistep process of metastasis, different cellular functions are influenced by urokinase. The enzyme is known to be effective via both proteolytical and signal transduction me...

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Published inInternational journal of cancer Vol. 77; no. 1; pp. 153 - 160
Main Authors Haeckel, Carsten, Krueger, Sabine, Roessner, Albert
Format Journal Article
LanguageEnglish
Published New York Wiley Subscription Services, Inc., A Wiley Company 03.07.1998
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Abstract Expression of urokinase‐type plasminogen activator (u‐PA) strongly correlates with a malignant tumor cell phenotype. In the multistep process of metastasis, different cellular functions are influenced by urokinase. The enzyme is known to be effective via both proteolytical and signal transduction mechanisms. In the present study, the osteosarcoma cell line MNNG/HOS was transfected with a vector capable of expressing an antisense transcript, complementary to 1,021 bases of the 3′ end of u‐PA cDNA. This construct was most effective in reducing u‐PA expression in previous experiments. Stably transfected antisense (as) cell lines were characterized and compared with the parental MNNG/HOS. Antisense transfection of MNNG/HOS gave the following results: (1) stable incorporation of the construct into the genome of as‐clones, as detected by Southern blot analysis; (2) decreased mRNA level of u‐PA, as detected by Northern blot analysis; (3) approximately 50% reduced enzyme expression in cell culture medium and cell homogenate; and (4) unchanged cellular proliferation activity and u‐PAR expression. In further functional analysis, as‐clones showed (1) significantly reduced invasion and motility in modified Transwell chambers (random migration and chemotaxis with collagen I as a chemoattractant); (2) significantly reduced adhesion on matrices of collagen I and vitronectin; (3) unchanged adhesion properties on Matrigel matrix; and (4) reduced metastatic potential to lungs and especially liver in chick embryos after i.v. infection into chorioallantoic membrane veins. Our data show that in MNNG/HOS urokinase influences cellular malignancy by promoting migration and selective adhesion. These specific functions were notable in addition to the effects on invasion and basement membrane degradation. Int. J. Cancer 77:153–160, 1998.© 1998 Wiley‐Liss, Inc.
AbstractList Expression of urokinase-type plasminogen activator (u-PA) strongly correlates with a malignant tumor cell phenotype. In the multistep process of metastasis, different cellular functions are influenced by urokinase. The enzyme is known to be effective via both proteolytical and signal transduction mechanisms. In the present study, the osteosarcoma cell line MNNG/HOS was transfected with a vector capable of expressing an antisense transcript, complementary to 1,021 bases of the 3' end of u-PA cDNA. This construct was most effective in reducing u-PA expression in previous experiments. Stably transfected antisense (as) cell lines were characterized and compared with the parental MNNG/HOS. Antisense transfection of MNNG/HOS gave the following results: (1) stable incorporation of the construct into the genome of as-clones, as detected by Southern blot analysis; (2) decreased mRNA level of u-PA, as detected by Northern blot analysis; (3) approximately 50% reduced enzyme expression in cell culture medium and cell homogenate; and (4) unchanged cellular proliferation activity and u-PAR expression. In further functional analysis, as-clones showed (1) significantly reduced invasion and motility in modified Transwell chambers (random migration and chemotaxis with collagen I as a chemoattractant); (2) significantly reduced adhesion on matrices of collagen I and vitronectin; (3) unchanged adhesion properties on Matrigel matrix; and (4) reduced metastatic potential to lungs and especially liver in chick embryos after i.v. infection into chorioallantoic membrane veins. Our data show that in MNNG/HOS urokinase influences cellular malignancy by promoting migration and selective adhesion. These specific functions were notable in addition to the effects on invasion and basement membrane degradation.
Expression of urokinase‐type plasminogen activator (u‐PA) strongly correlates with a malignant tumor cell phenotype. In the multistep process of metastasis, different cellular functions are influenced by urokinase. The enzyme is known to be effective via both proteolytical and signal transduction mechanisms. In the present study, the osteosarcoma cell line MNNG/HOS was transfected with a vector capable of expressing an antisense transcript, complementary to 1,021 bases of the 3′ end of u‐PA cDNA. This construct was most effective in reducing u‐PA expression in previous experiments. Stably transfected antisense (as) cell lines were characterized and compared with the parental MNNG/HOS. Antisense transfection of MNNG/HOS gave the following results: (1) stable incorporation of the construct into the genome of as‐clones, as detected by Southern blot analysis; (2) decreased mRNA level of u‐PA, as detected by Northern blot analysis; (3) approximately 50% reduced enzyme expression in cell culture medium and cell homogenate; and (4) unchanged cellular proliferation activity and u‐PAR expression. In further functional analysis, as‐clones showed (1) significantly reduced invasion and motility in modified Transwell chambers (random migration and chemotaxis with collagen I as a chemoattractant); (2) significantly reduced adhesion on matrices of collagen I and vitronectin; (3) unchanged adhesion properties on Matrigel matrix; and (4) reduced metastatic potential to lungs and especially liver in chick embryos after i.v. infection into chorioallantoic membrane veins. Our data show that in MNNG/HOS urokinase influences cellular malignancy by promoting migration and selective adhesion. These specific functions were notable in addition to the effects on invasion and basement membrane degradation. Int. J. Cancer 77:153–160, 1998.© 1998 Wiley‐Liss, Inc.
Author Krueger, Sabine
Roessner, Albert
Haeckel, Carsten
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Issue 1
Keywords Human
u-Plasminogen activator
Serine endopeptidases
Enzyme
Pathogenesis
Diseases of the osteoarticular system
Enzyme inhibitor
Antisense RNA
Malignant tumor
Metastasis
Basement membrane
Degradation
Peptidases
Osteosarcoma
Dissemination
Established cell line
Hydrolases
Bone
Language English
License CC BY 4.0
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PublicationTitle International journal of cancer
PublicationTitleAlternate Int J Cancer
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Wiley-Liss
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Snippet Expression of urokinase‐type plasminogen activator (u‐PA) strongly correlates with a malignant tumor cell phenotype. In the multistep process of metastasis,...
Expression of urokinase-type plasminogen activator (u-PA) strongly correlates with a malignant tumor cell phenotype. In the multistep process of metastasis,...
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StartPage 153
SubjectTerms Animals
Biological and medical sciences
Bone Neoplasms - genetics
Bone Neoplasms - pathology
Cell Division - drug effects
Chick Embryo
Dissemination
Gene Expression Regulation, Neoplastic
Humans
Medical sciences
Neoplasm Invasiveness
Oligonucleotides, Antisense - administration & dosage
Oligonucleotides, Antisense - genetics
Osteosarcoma - genetics
Osteosarcoma - pathology
Tumor cell
Tumor Cells, Cultured
Tumors
Urokinase-Type Plasminogen Activator - antagonists & inhibitors
Urokinase-Type Plasminogen Activator - genetics
Title Antisense inhibition of urokinase: Effect on malignancy in a human osteosarcoma cell line
URI https://onlinelibrary.wiley.com/doi/abs/10.1002%2F%28SICI%291097-0215%2819980703%2977%3A1%3C153%3A%3AAID-IJC23%3E3.0.CO%3B2-E
https://www.ncbi.nlm.nih.gov/pubmed/9639407
https://search.proquest.com/docview/17564738
https://search.proquest.com/docview/79952882
Volume 77
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