Tumor Biology Before and After Surgery

I did not get new pathology report on my original tumor after my BMX. They just referred to the original biopsy. After chemo there were only "rare" cells that remained so maybe that would make it harder. They did a path work up on the "surprise" tumor in the other breast though. Different makeup on that one.

I received a pathology report from my double mastectomy. The pathology report was different from the biopsy report.

What type of pathology is performed on post-surgical tissue if often dependent on what is determined at the biopsy. If you have surgery for what is thought to be DCIS based on biopsy, the post-surgical tissue will be looked at carefully to double check for any invasive element because that could potentially change treatment. At my biopsy it was determined that based on the core samples I was strongly ER+ and strongly Her2+, so there wasn't much need to repeat testing for Her2 or hormonal receptors on my post-surgical tissue. I also had Mammaprint testing done on a biopsy core sample so there was a pre-surgical double check of hormonal and Her2. A pathology report was generated after surgery regarding the IDC tumor size in entirety, my bi-lat SNB, the cored nipples since I had skin and nipple sparing surgery, my supposedly prophylactic left breast tissue was checked, which contained surprise ADH and ALH, and the extent of DCIS was noted in addition to the IDC on the cancer side because it had not previously been quantified by size since it was not seen on imaging. For those who are ER+ and have OncotypeDx testing done, a double check of hormonal receptor and Her2 status comes by way of that result. If hormonal receptors have low percentages, or Her2 is equivocal, I think testing for these is sometimes done post-surgically if it has not been tested again on core samples prior to surgery. Generally, if there is potential to find something that changes treatment, repeat testing is done, but I don't think that aspect is routine post-surgically.

Hi SummerAngel:

In my case, I had a surgical excisional biopsy on the left. The DCIS in the surgical biopsy was tested for ER and PR status. ER and PR testing was not repeated on the DCIS in the left mastectomy sample (MGH, 2013).

While each biopsy, surgical sample, or re-excision must be assessed by the pathologist and summarized in a written report, the question of retesting appears to be fact-dependent.

The results of ER, PR and HER2 testing on biopsy tissue are generally considered sufficiently accurate for the purpose of prescribing neoadjuvant chemotherapy in, for example, HER2-positive or triple-negative invasive disease. Note that those with pathologic complete responses cannot be retested.

Where neoadjuvant treatment is not received, with invasive disease, re-testing for HER2 status is not always repeated. However, there are situations where guidelines recommend repeat testing on surgically-removed tissues. See for example:

>> Wolff (2013) (ASCO/CAP Guideline Update): "Recommendations for Human Epidermal Growth Factor Receptor 2 Testing in Breast Cancer: American Society of Clinical Oncology/College of American Pathologists Clinical Practice Guideline Update"

>> http://ascopubs.org/doi/pdf/10.1200/jco.2013.50.9984

>> "In summary, if available, perform the first test in the core biopsy specimen in a patient with newly diagnosed breast cancer. If the test result is clearly positive or clearly negative as defined in Table 1, no retesting is needed. If the test is negative and there is apparent histopathologic discordance (Table 2), or if specimen handling has not been in accordance with guideline recommendations, a section of the tumor from the excisional specimen should be tested. If this result is positive, no further testing is needed. However, if the test is negative and there remains significant clinical concern about the result after consultation between the pathologist and the medical oncologist, it may be appropriate to repeat the test in a different block from the patient's tumor. If all three tests are negative, no additional testing is recommended."

The above may not be a comprehensive summary of all situations in which a pathologist may retest.

Here is a link to the 2010 ASCO/CAP guideline for ER and PR testing. If you search the pdf document for the word "repeat" or "biopsy", you can see some of the considerations relevant to the question of repeat testing of either the same sample, a different block, or a different specimen.

>> Hammond (2010)( ASCO/CAP Guideline): "American Society of Clinical Oncology/College of American Pathologists Guideline Recommendations for Immunohistochemical Testing of Estrogen and Progesterone Receptors in Breast Cancer"

>> https://www.asco.org/sites/new-www.asco.org/files/content-files/practice-and-guidelines/documents/2010-JCO-ASCO-CAP-Immunohistochemical-testing.full_.pdf

This may not be a comprehensive summary of all situations in which a pathologist may retest.

While not a "retest" but in fact a new test, I note that if a biopsy shows pure DCIS (tested for ER and PR), but an area of invasive breast cancer is later identified in surgical samples, the invasive breast cancer should be tested for all three ER, PR and HER2 statuses, no matter how small (if feasible).

BarredOwl

[[[EDIT (03 June 2018): Please note this 2018 ASCO Focused Guideline Update for HER2 testing:

Wolff (2018): "Human Epidermal Growth Factor Receptor 2 Testing in Breast Cancer: American Society of Clinical Oncology/College of American Pathologists Clinical Practice Guideline Focused Update"

http://ascopubs.org/doi/pdf/10.1200/JCO.2018.77.8738 ]]]

Summer Angel, I was just looking at your stats. Did you not have radiation or chemo?

When I had my BMX my clean breast was found to have 9mm IDC/DCIS. I am on tumor board discussions today but right now the plan is no radiation on that side. RO said if I had had just a lumpectomy there would be chemo but since I had a BMX no rads were needed. Just curious as to others treatments. I already did preadjuvent chemo and will be in tamoxifen after rads to my original known cancer side

I have the results from both my biopsy and my lumpectomy. There were 2 results which were slightly different. The pr was 100% on 1 test and 99.89% on the other so that is essentially the same. The Ki67 was 3.3% on the biopsy and 10% on the lumpectomy. I have read that the biopsy damage itself causes the numbers to go up on the Ki67 for later surgery. Some tend to believe that the biopsy result is more accurate because of this but others say that Ki67 testing varies greatly and is not reliable. Use plain text editor

Reviving a month old post I just noticed, my core needle biopsy showed hormone receptor negative, but HER2 positive results. Against medical advice, I refused targeted (Perjeta Herceptin) & chemotherapy and moved forward with a lumpectomy. The lumpectomy / solid tumor pathology report also showed hormone receptor negative; however, to my dismay, it showed HER2 negative or a triple negative diagnosis.

Was the core needle sample not representative of the entire tumor? Did the tumor morph to triple negative in Lee's than two months? No idea. With the poorer prognosis associated with triple negative cancer, I ended up reluctantly doing AC + T chemo. Are there HER2+ cells migrating through my system? I don't know. My first mammogram and two post-chemo biomarker tests showed nothing worrisome plus a tiny nodule in my lung discovered during a baseline chest CT scan hasn't grown so I'm hopeful that the cancer won't metastasize or recur. Also, nothing disturbing was found during a recent reduction surgery. I personally would want pathology tests every step of the way.

Lyn

Interesting, Leatherette. DCIS was found in the margins of my first lumpectomy so I had to have more tissue removed two weeks later.

Lyn

i wasn't retested as i had a PCR, but interestingly, i had 2 biopsies leading to 3 different path reports (two of them from the same biopsy but different slides). her2 status was consistent over the three reports but grade wasn't and pr/er % are wildly different.

medicine is not a hard science!