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-   -   How many ER+ PR- are there? (https://her2support.org/vbulletin/showthread.php?t=42288)

Jean 12-05-2009 08:43 PM
How many ER+ PR- are there?
 
Lani posted recently about ER+ verses ER- relapse time.
Becky posed that ER+ PR- is a rare group.
I am just curious how many of us are ER+ PR- if you don't mind....

ROLL CALL...(LOL)

Thanks,
Jean

BonnieR 12-05-2009 09:31 PM
Re: How many ER+ PR- are there?
 
I am in this select group.

PinkGirl 12-05-2009 09:45 PM
Re: How many ER+ PR- are there?
 
I am too ... and I like being weird :)

freyja 12-05-2009 09:47 PM
Re: How many ER+ PR- are there?
 
Here! Er+ pr- her2+++

Becky 12-05-2009 10:22 PM
Re: How many ER+ PR- are there?
 
I am weird too

bejuce 12-06-2009 12:38 AM
Re: How many ER+ PR- are there?
 
Same here...

Chelee 12-06-2009 12:42 AM
Re: How many ER+ PR- are there?
 
Actually...I'm not sure if I count official...but my recent biopsy report from femur said I'm Er + and Pr -.

Orignal dx I was weakly Er & Pr. So you choose which one I am. lol

I think this qualifies me for the "weird" group. :)

Chelee

DianeH 12-06-2009 12:33 PM
Re: How many ER+ PR- are there?
 
I am also ER+ and PR-....

Patb 12-06-2009 04:03 PM
Re: How many ER+ PR- are there?
 
I am ER+ 90 percent, PR-
Really wierd
patb

PinkGirl 12-06-2009 04:46 PM
Re: How many ER+ PR- are there?
 

You're officially weird Chelee! It's actually easier to be weird than
it is to be normal .... you do something weird and everyone just
says ... "oh, she's always weird" .... makes life easier for me. :)

Nancy L 12-06-2009 05:27 PM
Re: How many ER+ PR- are there?
 
Chelee's response is important to remember and a reminder that everytime we are rediagnosed, it is very important to get the tumor reevaluated. Receptor status and Her2 status can change during your journey. I just went through serious surgery to get a surgical biopsy completed in a very difficult spot in my neck because Dr. Slamon said it wasn't enough to know it was breast cancer----he needed to know all the characteristics of my recurrence in the neck to know exactly how to treat me. It wasn't until the past few years that they discovered tumors can change characteristics.

Jackie07 12-06-2009 10:41 PM
Re: How many ER+ PR- are there?
 
ER+ (weakly) PR- both times*. Have had almost 5 years of Tamoxifen. Will discuss options with Onco soon.

Correction: Oncology nurse just called me back - turned out my recurrence is ER -. How about that, he hid the news from me just so he could get me to take 5 years worth of Tamoxifen without getting probed by me... Yet I've continued my questioning regardless... :)

SuThorn 12-07-2009 10:22 AM
Re: How many ER+ PR- are there?
 
I am also in the weird group. ER+/PR-...

Thanks, Suzanne

Barbara2 12-14-2009 10:53 AM
Re: How many ER+ PR- are there?
 
Me, too...ER+, Pr-.

krisvell 12-14-2009 06:56 PM
Re: How many ER+ PR- are there?
 
You can add me to the list.

Hopeful 12-15-2009 07:54 AM
Re: How many ER+ PR- are there?
 
Jean, et al - an interesting abstract from SABCS for you: http://her2support.org/vbulletin/sho...eferrerid=1173

Hopeful

Jean 12-17-2009 07:57 PM
Re: How many ER+ PR- are there?
 
Thank you Hopeful, as always you are a great researcher. Knowing that the er+ pr- was a subtype
that is unique...now after reading the post there is another level to this...very intersting. Do you know of any other articles or posting?

Yes we are certainly a bunch of weirdo's!!! lol

thanks all,
Jean

DarleneM 12-17-2009 08:07 PM
Re: How many ER+ PR- are there?
 
I'm in...although only weakly ER+

Jackie07 12-18-2009 09:16 AM
Re: How many ER+ PR- are there?
 
This study was presented in the ASCO meeting in 2008. Don't know if (most likely) it's been posted. Thought it might be relavant in the discussion here. It shows the Er, Pr, and/or Her2 status can change in relapsed breast cancer.

***************************

J Clin Oncol 26: 2008 (May 20 suppl; abstr 1000)


Author(s):
R. MacFarlane, C. Speers, H. Masoudi, S. Chia

Abstract:

Background: Relapsed/metastatic breast cancers are presumed to have the same predictive factors as the initial primary tumour. As such, the majority of patients do not have additional biopsies performed at the time of relapse. Recent small studies have suggested that a significant proportion of relapsed lesions may have a change in the hormone receptor and/or HER2 receptor status from the original tumour. We sought to compare the hormonal and HER2 receptor status of relapsed/metastatic breast cancer tumours with those of the original tumour from a large population-based database and tissue microarray (TMA) cohort. Methods: Using the BCCA Breast Cancer Outcomes Unit Database from 1986-1992, patients with biopsy proven relapses were identified. These identified patients were linked to a current large TMA series (n=4,444) of primary breast cancers. Charts were reviewed, and available tissue blocks of the relapsed/metastatic cancer were requested and collected. An additional TMA was created of the relapsed/metastatic tumours. IHC was performed for ER (LabVision SP 1 antibody), PR (Ventana 1E2 antibody) and HER2 (LabVision SP 3 antibody) on both the primary and relapsed tumours. The pathologist was blinded to knowledge of the primary tumour receptor status. Results: 281 cases were linked between the BCOU database and the TMA series. Of the 281 cases, 184 tissue blocks were received, and 160 had adequate tumour for analyses. Of the 160 blocks, 115 (72%) had no changes in either the ER/ PR or HER2 status. Of the 45 (28%) tumours that did have changes in the receptor status, 11 (7%) were local recurrence, 34 (21%) were regional or distant relapses. Among the 34 regional/distant relapses 11 went from ER/PR(+) to ER/PR(-), 14 went from ER/PR(-) to ER/PR(+), 3 went from HER2(-) to HER2(+), and 6 went from HER2(+) to HER2(-). Conclusions: This is one of the largest known studies assessing for changes in molecular phenotype between the primary and relapsed breast cancer. A significant proportion (21%) of relapsed tumours had changes in either ER/PR or HER2 receptor status. This study suggests that biopsies of relapsed/metastatic breast cancers should be performed routinely.

Jackie07 12-18-2009 09:30 AM
Re: How many ER+ PR- are there?
 
And here's the advice I got from my 2nd Sister-in-law's bc oncologist (in Taiwan):

Since your breast cancer is ER (+), although the percentage of ER is 5-10%. Hormonal therapy with tamoxifen or AI (arimidex) is the treatment of choice.

The disadvantage of tamoxifen: Uterine myoma, uterine carcinoma...etc. but less osteroporosis.
The disadvantage of arimidex (AI analogue): severe osteroporosis..

Conventionally, chemotherapy will destroy the ovarian functions, oophorectomy, therefore, is not necessroy.
But if you still have menstration indicating the normal ovary function, oophorectomy and hysterectomy (to avoid uterine tumors) followed by
tamoxifen treatment are treatments of choice.

According to your questions below, my answer is:

If you have still menstration now, surgical removal of ovary and uterus is advised, provided chemotherapy did not destroy ovary functions.
Both tamoxifen for 5 years and tamoxifen 2 years followed by arimidex 3 years are fine for your condition.

*****************************************


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