Inhibition of Spontaneous Rat Osteosarcoma Lung Metastasis by 3 S ‐[4‐(Nhydroxyamino)‐2 R ‐isobutylsuccinyl]amino‐1‐methoxy‐3,4‐dihydrocarbostyril, a Novel Matrix Metalloproteinase Inhibitor

Inhibition of Spontaneous Rat Osteosarcoma Lung Metastasis by 3 S ‐[4‐(Nhydroxyamino)‐2 R ‐isobutylsuccinyl]amino‐1‐methoxy‐3,4‐dihydrocarbostyril, a Novel Matrix Metalloproteinase Inhibitor

In the present experiment, we examined the effects of OPB‐3206, 3S‐[4‐(N‐hydroxyamino)‐2R isobutylsuccinyl] amino‐1‐methoxy‐3,4‐dihydrocarbostyril, a novel metalloproteinase inhibitor, on the growth and metastasis of transplantable osteosarcomas (spontaneous osteosarcoma, selected lung metastatic le...

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Veröffentlicht in:Cancer science 1999-03, Vol.90 (3)
Hauptverfasser: Kido, Akira, Tsutsumi, Masahiro, Iki, Katsumichi, Motoyama, Masaaki, Takahama, Makoto, Tsujiuchi, Toshifumi, Morishita, Toru, Tatsumi, Kunihiko, Tamai, Susumu, Konishi, Yoichi
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Sprache:eng
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Bone cancer
Collagen
Collagenase
Interstitial collagenase
Lung nodules
Matrix metalloproteinase
Metalloproteinase
Metastases
Metastasis
Oral administration
Osteosarcoma
Stromelysin
Tumors
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container_issue 3
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container_title Cancer science
container_volume 90
creator Kido, Akira
Tsutsumi, Masahiro
Iki, Katsumichi
Motoyama, Masaaki
Takahama, Makoto
Tsujiuchi, Toshifumi
Morishita, Toru
Tatsumi, Kunihiko
Tamai, Susumu
Konishi, Yoichi
description In the present experiment, we examined the effects of OPB‐3206, 3S‐[4‐(N‐hydroxyamino)‐2R isobutylsuccinyl] amino‐1‐methoxy‐3,4‐dihydrocarbostyril, a novel metalloproteinase inhibitor, on the growth and metastasis of transplantable osteosarcomas (spontaneous osteosarcoma, selected lung metastatic lesions; S‐SLM), which were previously established in rats. OPB‐3206 inhibited the activities of interstitial collagenase, gelatinases A and B, and stromelysin in vitro. After oral administration to rats, its serum concentration peaked at 40 min and the drug was no longer detectable at 8 h. When OPB‐3206 was orally administered at 0%, 0.1% and 0.4% in the diet for 4 weeks, starting 7 days after subcutaneous transplantation of osteosarcomas to male Fischer 344 rats, numbers of lung metastatic nodules were significantly reduced by the highest dose, while the growth of subcutaneous tumors was not affected. Zymographic analysis showed the presence of pro matrix metalloproteinase (proMMP)‐2, proMMP‐9 and MMP‐9 activities in S‐SLM. In animals fed 0.4% OPB‐3206, the activity of proMMP‐9 was increased, but that for MMP‐9 had become undetectable. The results thus suggest that OPB‐3206 selectively inhibits lung metastasis of rat transplantable osteosarcomas by inhibiting MMP‐9 activation.
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OPB‐3206 inhibited the activities of interstitial collagenase, gelatinases A and B, and stromelysin in vitro. After oral administration to rats, its serum concentration peaked at 40 min and the drug was no longer detectable at 8 h. When OPB‐3206 was orally administered at 0%, 0.1% and 0.4% in the diet for 4 weeks, starting 7 days after subcutaneous transplantation of osteosarcomas to male Fischer 344 rats, numbers of lung metastatic nodules were significantly reduced by the highest dose, while the growth of subcutaneous tumors was not affected. Zymographic analysis showed the presence of pro matrix metalloproteinase (proMMP)‐2, proMMP‐9 and MMP‐9 activities in S‐SLM. In animals fed 0.4% OPB‐3206, the activity of proMMP‐9 was increased, but that for MMP‐9 had become undetectable. 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The results thus suggest that OPB‐3206 selectively inhibits lung metastasis of rat transplantable osteosarcomas by inhibiting MMP‐9 activation.</description><subject>Bone cancer</subject><subject>Collagen</subject><subject>Collagenase</subject><subject>Interstitial collagenase</subject><subject>Lung nodules</subject><subject>Matrix metalloproteinase</subject><subject>Metalloproteinase</subject><subject>Metastases</subject><subject>Metastasis</subject><subject>Oral administration</subject><subject>Osteosarcoma</subject><subject>Stromelysin</subject><subject>Tumors</subject><issn>1347-9032</issn><issn>1349-7006</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>1999</creationdate><recordtype>article</recordtype><sourceid>ABUWG</sourceid><sourceid>AFKRA</sourceid><sourceid>AZQEC</sourceid><sourceid>BENPR</sourceid><sourceid>CCPQU</sourceid><sourceid>DWQXO</sourceid><sourceid>GNUQQ</sourceid><recordid>eNqNUF1KAzEQXkTB-nOHAV8UWtjdLC15FkXBVmh9EynZbeqmZDM1M5HmzSN4Mg_hSUyXHkCYP-b75mNmjrJBISo5muT5-LivJyOZi_I0OyPa5LkYV7IaZD-PrjW1YYMOcA2LLTpWTmMgmCuGZ2KNpHyDnYKn4N5hqllRMkNQRxCwgN-v79cqhetZG1ced1F1xuFN6pQw36OGsA4cLYWmMS7at56QgCJ5p7lNM6kSw73KyvQqjfI1Ekdv7BAUzPBTW5gq9mbXr2Atbj2yNk6RhsMR6C-yk7WypC8P-Ty7ur97uX0YJfJH0MTLDQbvErQshZSFlOkL4n-sP3cAdsc</recordid><startdate>19990301</startdate><enddate>19990301</enddate><creator>Kido, Akira</creator><creator>Tsutsumi, Masahiro</creator><creator>Iki, Katsumichi</creator><creator>Motoyama, Masaaki</creator><creator>Takahama, Makoto</creator><creator>Tsujiuchi, Toshifumi</creator><creator>Morishita, Toru</creator><creator>Tatsumi, Kunihiko</creator><creator>Tamai, Susumu</creator><creator>Konishi, Yoichi</creator><general>John Wiley &amp; 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S‐SLM), which were previously established in rats. OPB‐3206 inhibited the activities of interstitial collagenase, gelatinases A and B, and stromelysin in vitro. After oral administration to rats, its serum concentration peaked at 40 min and the drug was no longer detectable at 8 h. When OPB‐3206 was orally administered at 0%, 0.1% and 0.4% in the diet for 4 weeks, starting 7 days after subcutaneous transplantation of osteosarcomas to male Fischer 344 rats, numbers of lung metastatic nodules were significantly reduced by the highest dose, while the growth of subcutaneous tumors was not affected. Zymographic analysis showed the presence of pro matrix metalloproteinase (proMMP)‐2, proMMP‐9 and MMP‐9 activities in S‐SLM. In animals fed 0.4% OPB‐3206, the activity of proMMP‐9 was increased, but that for MMP‐9 had become undetectable. 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subjects Bone cancer
Collagen
Collagenase
Interstitial collagenase
Lung nodules
Matrix metalloproteinase
Metalloproteinase
Metastases
Metastasis
Oral administration
Osteosarcoma
Stromelysin
Tumors
title Inhibition of Spontaneous Rat Osteosarcoma Lung Metastasis by 3 S ‐[4‐(Nhydroxyamino)‐2 R ‐isobutylsuccinyl]amino‐1‐methoxy‐3,4‐dihydrocarbostyril, a Novel Matrix Metalloproteinase Inhibitor
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