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Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates

To elucidate tumor progression‐enhancing factor(s), we examined the effects of host inflammation and host immunological status on in vivo tumor progression. One × 10(4) cells of QR clones (QR‐32, ‐20 and ‐18), regressor tumor clones of 3‐methylcholanthrene‐induced fibrosarcoma, were unable to grow w...

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Autores principales: Okada, Futoshi, Hosokawa, Masuo, Hamada, Jun‐ichi, Hasegawa, Junji, Mizutani, Masatoshi, Takeichi, Noritoshi, Kobayashi, Hiroshi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 1993
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5919104/
https://www.ncbi.nlm.nih.gov/pubmed/8294213
http://dx.doi.org/10.1111/j.1349-7006.1993.tb02827.x
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author Okada, Futoshi
Hosokawa, Masuo
Hamada, Jun‐ichi
Hasegawa, Junji
Mizutani, Masatoshi
Takeichi, Noritoshi
Kobayashi, Hiroshi
author_facet Okada, Futoshi
Hosokawa, Masuo
Hamada, Jun‐ichi
Hasegawa, Junji
Mizutani, Masatoshi
Takeichi, Noritoshi
Kobayashi, Hiroshi
author_sort Okada, Futoshi
collection PubMed
description To elucidate tumor progression‐enhancing factor(s), we examined the effects of host inflammation and host immunological status on in vivo tumor progression. One × 10(4) cells of QR clones (QR‐32, ‐20 and ‐18), regressor tumor clones of 3‐methylcholanthrene‐induced fibrosarcoma, were unable to grow when injected s.c. into C57BL/6 mice in cell suspension form. However, QR clones grew and were lethal when s.c. implanted, attached to plastic plates. Furthermore, the tumor lines (QRpP) obtained from the tumors which had arisen from the plate‐attached QR‐32 clone cells no longer required plastic plates for their growth in normal mice, and had acquired stable malignant phenotypes. Although QR‐32 cells became lethal when injected at the site of plastic plate implantation 1, 5 and 10 days before tumor injection, few tumors developed when plastic plates had been implanted 20 or 30 days before tumor injection. We established culture clones from the tumors arising in normal mice and mice immunosuppressed by irradiation. Clones derived from the tumors which had arisen in normal mice after implantation with plastic plates were lethal when re‐implanted in normal mice (71%). On the other hand, clones derived from the tumors that arose in irradiated mice with or without plastic plates were lethal in only a few normal mice, when re‐implanted (20 and 8%, respectively). These results indicate that QR clone cell progression is enhanced by the early phase of inflammation at the site of plastic plate implantation and that the progression‐enhancing activity of co‐implantation with a plastic plate is inhibited by previous whole‐body irradiation of hosts.
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spelling pubmed-59191042018-05-11 Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates Okada, Futoshi Hosokawa, Masuo Hamada, Jun‐ichi Hasegawa, Junji Mizutani, Masatoshi Takeichi, Noritoshi Kobayashi, Hiroshi Jpn J Cancer Res Article To elucidate tumor progression‐enhancing factor(s), we examined the effects of host inflammation and host immunological status on in vivo tumor progression. One × 10(4) cells of QR clones (QR‐32, ‐20 and ‐18), regressor tumor clones of 3‐methylcholanthrene‐induced fibrosarcoma, were unable to grow when injected s.c. into C57BL/6 mice in cell suspension form. However, QR clones grew and were lethal when s.c. implanted, attached to plastic plates. Furthermore, the tumor lines (QRpP) obtained from the tumors which had arisen from the plate‐attached QR‐32 clone cells no longer required plastic plates for their growth in normal mice, and had acquired stable malignant phenotypes. Although QR‐32 cells became lethal when injected at the site of plastic plate implantation 1, 5 and 10 days before tumor injection, few tumors developed when plastic plates had been implanted 20 or 30 days before tumor injection. We established culture clones from the tumors arising in normal mice and mice immunosuppressed by irradiation. Clones derived from the tumors which had arisen in normal mice after implantation with plastic plates were lethal when re‐implanted in normal mice (71%). On the other hand, clones derived from the tumors that arose in irradiated mice with or without plastic plates were lethal in only a few normal mice, when re‐implanted (20 and 8%, respectively). These results indicate that QR clone cell progression is enhanced by the early phase of inflammation at the site of plastic plate implantation and that the progression‐enhancing activity of co‐implantation with a plastic plate is inhibited by previous whole‐body irradiation of hosts. Blackwell Publishing Ltd 1993-12 /pmc/articles/PMC5919104/ /pubmed/8294213 http://dx.doi.org/10.1111/j.1349-7006.1993.tb02827.x Text en
spellingShingle Article
Okada, Futoshi
Hosokawa, Masuo
Hamada, Jun‐ichi
Hasegawa, Junji
Mizutani, Masatoshi
Takeichi, Noritoshi
Kobayashi, Hiroshi
Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates
title Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates
title_full Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates
title_fullStr Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates
title_full_unstemmed Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates
title_short Progression of a Weakly Tumorigenic Mouse Fibrosarcoma at the Site of Early Phase of Inflammation Caused by Plastic Plates
title_sort progression of a weakly tumorigenic mouse fibrosarcoma at the site of early phase of inflammation caused by plastic plates
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5919104/
https://www.ncbi.nlm.nih.gov/pubmed/8294213
http://dx.doi.org/10.1111/j.1349-7006.1993.tb02827.x
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