Estradiol induced changes in tumor growth and steroid receptor content in a heterotransplanted human endometrial adenocarcinoma

Horvath, G; Fernö, Mårten; Baldetorp, Bo; Cameron, R; Ranstam, Jonas

Estradiol induced changes in tumor growth and steroid receptor content in a heterotransplanted human endometrial adenocarcinoma

Mark

Horvath, G ; Fernö, Mårten ^LU ; Baldetorp, Bo ^LU ; Cameron, R and Ranstam, Jonas ^LU (1991) In In Vivo 5(4). p.401-406

Abstract: To study the importance of estrogen availability to growth pattern and other tumor characteristic such as estrogen receptor (ER) and progesterone receptor (PgR) content and histopathology, we have used a human tumor-nude mouse model, in which an ER- and PgR-positive and estradiol-sensitive (stimulated) human endometrial adenocarcinoma was heterotransplanted and serially passed in female (non-oophorectomized) nude mice over a period of one year. Pieces from this tumor were transplanted into oophorectomized nude mice, randomly divided into two groups, one with and one without estradiol treatment (preparation phase). After four weeks, pieces from both these groups were again transplanted into oophorectomized nude mice, each group being... (More); To study the importance of estrogen availability to growth pattern and other tumor characteristic such as estrogen receptor (ER) and progesterone receptor (PgR) content and histopathology, we have used a human tumor-nude mouse model, in which an ER- and PgR-positive and estradiol-sensitive (stimulated) human endometrial adenocarcinoma was heterotransplanted and serially passed in female (non-oophorectomized) nude mice over a period of one year. Pieces from this tumor were transplanted into oophorectomized nude mice, randomly divided into two groups, one with and one without estradiol treatment (preparation phase). After four weeks, pieces from both these groups were again transplanted into oophorectomized nude mice, each group being randomly allocated to two subgroups, one with and one without estradiol treatment (experimental phase). Tumor growth was measured during the experimental phase, whereas both ER and PgR content and histopathology were analyzed after the experimental phase. Our findings indicate that even short-term growth under estradiol-poor conditions can trigger such progressive changes as reduced steroid receptor content, development of a less differentiated tumor and tendency to enhanced tumor growth. On the other hand, estradiol-rich conditions enhanced ER activation, PgR induction and tumor differentiation in the same tumor line. The estrogenic conditions under which a tumor grows may thus be crucial determinants of tumor progression. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1105650

author

Horvath, G ; Fernö, Mårten ^LU ; Baldetorp, Bo ^LU ; Cameron, R and Ranstam, Jonas ^LU

organization

publishing date

1991

type

Contribution to journal

publication status

published

subject

Cancer and Oncology

in

In Vivo

volume

5

issue

4

pages

401 - 406

publisher

In vivo

external identifiers

pmid:1810429
scopus:0025983224

ISSN

0258-851X

language

English

LU publication?

yes

id

77999bb9-4a48-457a-baf7-b204a1dfe2ad (old id 1105650)

date added to LUP

2016-04-01 15:48:36

date last changed

2021-01-03 05:40:00

@article{77999bb9-4a48-457a-baf7-b204a1dfe2ad,
  abstract     = {{To study the importance of estrogen availability to growth pattern and other tumor characteristic such as estrogen receptor (ER) and progesterone receptor (PgR) content and histopathology, we have used a human tumor-nude mouse model, in which an ER- and PgR-positive and estradiol-sensitive (stimulated) human endometrial adenocarcinoma was heterotransplanted and serially passed in female (non-oophorectomized) nude mice over a period of one year. Pieces from this tumor were transplanted into oophorectomized nude mice, randomly divided into two groups, one with and one without estradiol treatment (preparation phase). After four weeks, pieces from both these groups were again transplanted into oophorectomized nude mice, each group being randomly allocated to two subgroups, one with and one without estradiol treatment (experimental phase). Tumor growth was measured during the experimental phase, whereas both ER and PgR content and histopathology were analyzed after the experimental phase. Our findings indicate that even short-term growth under estradiol-poor conditions can trigger such progressive changes as reduced steroid receptor content, development of a less differentiated tumor and tendency to enhanced tumor growth. On the other hand, estradiol-rich conditions enhanced ER activation, PgR induction and tumor differentiation in the same tumor line. The estrogenic conditions under which a tumor grows may thus be crucial determinants of tumor progression.}},
  author       = {{Horvath, G and Fernö, Mårten and Baldetorp, Bo and Cameron, R and Ranstam, Jonas}},
  issn         = {{0258-851X}},
  language     = {{eng}},
  number       = {{4}},
  pages        = {{401--406}},
  publisher    = {{In vivo}},
  series       = {{In Vivo}},
  title        = {{Estradiol induced changes in tumor growth and steroid receptor content in a heterotransplanted human endometrial adenocarcinoma}},
  volume       = {{5}},
  year         = {{1991}},
}

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Estradiol induced changes in tumor growth and steroid receptor content in a heterotransplanted human endometrial adenocarcinoma