ct scan report not good

Collins,
I'm sorry I have no exp. with Tamoxifin, but I'll say some prayers that they stop the disease from spreading and keep you comfortable.(((hugz)))..Joanne

Eleen,

I had been on tamoxifan from 13 June 2007 to 31 Aug 2007. It was a very easy chemo with no side effects. I took one tablet once a day and it gave my body time to recover from the toxic chemo regime I had been on. I was able to go on holidays for a few weeks. It kept my numbers stable until my body was able to commence doxil. I am due to have my third treatment of doxil tomorrow 14 Dec. Then a decision will be made if the doxil is working or if I have to switch to a different chemo. I also had 28 treatments of radium from 15 June 2005 until 17 August 2005. This is a long story and my present problems in relation to rental failure on 12 November were because of the radium. I am very slowly recovering from the renal failure but it has been a very slow recovery. I hope to feel much better in a weeks time and I am looking forward to a Happy and pain free Christmas. I will get back to you with the questions I should have asked, where I think we went wrong what happened to my CA125 etc. Irene.

Hormone treatments are fine - nothing to fear and very mild side-effects. Find out the exact hormone status of your cancer. It sounds as though it's definitely estrogen positive (ER+) but it could also be PR+ ie. a combination of both. If that's the case then you could also try this drug (in combination with tamoxifen) and as per with breast cancer no doubt both are better than one alone. If your cancer does not respond to tamoxifen then definitely try this one. The same drugs can be used for ovarian, uterine and breast cancers depending on hormone status. Mifepristone, however, is only available through the FMF's Compassionate Use Program:

Their website link is:
http://feminist.org/rrights/compassionateuse.asp


2003: Study of effect of mifepristone on apoptosis of human ovarian cancer cell line 3AO
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=retrieve&db=pubmed&list_uids=14728868&dopt=Abstract
• “Mifepristone inhibited significantly the proliferation and induced the cell apoptosis of cell line 3AO in dose-time dependent manner in vitro. The anti-tumor effect was related to down-regulation the expression of PR protein and bcl-2 protein, and to up-regulation the expression of p53 protein of 3AO cells.”

2003: Enhancement of antitumor effect of cisplatin against human ovarian carcinoma cells by mifepristone in vivo.
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=12651241&dopt=Abstract
• “At a non-toxic dose, RU486 may enhance the sensitivity of tumor cells to cisplatin in vivo, possibly through the mechanism of inhibiting GcS expression at the mRNA level.”

2004: Mifepristone Induces Growth Arrest, Caspase Activation, and Apoptosis of Estrogen Receptor-Expressing, Antiestrogen-Resistant Breast Cancer Cells
http://clincancerres.aacrjournals.org/cgi/content/abstract/10/15/5215
• “We demonstrate that: (a) estrogen receptor+progesterone receptor+, 4-OHT-resistant clonal variants can be isolated from an MCF-7 cell line in the absence of antiestrogen selection; and (b) MIF and MIF plus 4-OHT combination therapy induces growth arrest and active cell death of the antiestrogen-resistant breast cancer cells. These preclinical findings show potential for a combined hormonal regimen of an antiestrogen and an antiprogestin to combat the emergence of antiestrogen-resistant breast cancer cells and, ultimately, improve the therapeutic index of antiestrogen therapy.”