MammaPrint breast cancer test can help women avoid chemotherapy

News · 02-05-2013, 05:52 AM

The MammaPrint breast cancer test can dramatically reduce the number of women who need to undergo chemotherapy to treat the disease, according to a newly published study.

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gdpawel · 02-09-2013, 02:35 PM

Breast. 2011 Oct 1;20(3), S Paik

Abstract

Background:

There are five multi-gene expression based prognostic tests for breast cancer offered as reference lab tests - Mammaprint, MapQuant Dx, OncotypeDx, PAM50 Breast Cancer Intrinsic Subtype Classifier, and Theros Breast Cancer Index. Each claims to provide additional prognostic information beyond conventional prognostic markers and to aid in determining who should receive systemic therapy. Evidence for their clinical utility was reviewed to determine whether any of them should be considered as routine clinical test.

Methods:

Peer reviewed publications, meeting abstracts, and information provided by company web sites have been reviewed to compile information regarding their clinical utility according to the following criteria; (1) Analytical validity and regulatory approval of the reference lab test. (2) Level of evidence for clinical utility. (3) Whether published evidences support prognostic and/or predictive claim.

Results:

While published evidences for clinical claims for OncotypeDx and Mammaprint used reference lab tests, and the supporting evidences for other tests come from academic assays before being converted to reference lab tests, results from two large randomized clinical trials testing the clinical utility of OncotypeDx and Mammaprint are still several years away and until that time none of the markers would reach level I evidence by Marker Utility Grading System. However Oncotype Dx has reached a level IB evidence according to Simon modification to Marker Utility Grading System. Therefore OncotypeDx may be considered for routine clinical use as an adjunct to clinical and pathological information and has been incorporated into clinical guidelines in USA. While Mammaprint, MapQuantDx, and PAM50 have been repeatedly demonstrated to provide robust prognostic information, evidence for its worth as a predictive marker for chemotherapy benefit is yet to come from randomize clinical trials and therefore its utility is limited to prognostication. Meta-analysis of publicly available microarray based gene expression studies demonstrated that gene expression assays provide similar information and the most important information they provide is the proliferation activity. In untreated population, the prognostic impact of proliferation genes is limited to ER+HER2− subset since HER2+ or ER−HER2− subsets are associated with high proliferation activity. Therefore the clinical utility of these gene expression based tests is mainly for ER+HER2− subset. Since they are usually treated with adjuvant anti-estrogen therapies, for their clinical utility, demonstration of the interaction between the gene expression markers and chemotherapy in anti-estrogen treated cohort in a randomized clinical trial would be required. While OncoytpeDx is the only test supported by studies in a randomized clinical trial for adjuvant chemotherapy, other gene expression based tests are expected to provide similar information. Gene expression profiling assays as more reproducible and precise surrogates for tumor grade (MapQauntDx and Theros Breast Cancer Index) are very promising assays. However, absence of definitive predefined cut-off for defining the subset that benefit from chemotherapy validated in cohorts from randomized trials limit their clinical application.

http://www.thebreastonline.com/artic...301-0/abstract

gdpawel · 02-09-2013, 02:36 PM

Cary Presant, M.D.
Wilshire Oncology Medical Group

The decision of chemotherapy plus hormonal therapy versus hormonal therapy alone in patients with breast cancer, stage 1 or 2A is an important decision which we commonly make in our oncology practices. The advent of the Oncotype DX test, along with other similar tests such as MammaPrint and Mammostrat, have given us tools whose application is selectively very important. Recently, the adoption of gene expression profile testing has been reviewed by M. Hassett and coworkers (Journal of Clinical Oncology 30:2218-2226, 2012).

In over 7,000 women, 20% received gene expression profile testing. Of those who had the test, 50% received chemotherapy. The use of gene expression profiling became more common between 2006 and 2008 (increasing from 14.7% to 27.5%). Unfortunately, they did not have more up to date data in the past 4 years.

Needless to say, if an oncologist sees a clinical indication to use chemotherapy, addition of a gene expression profile test would be unnecessary. Similarly, if a patient were unwilling to consider chemotherapy, such a test would again be unnecessary. However, for women wanting the most appropriate, personalized, individualized therapy, the use of a gene expression profile test would be very important.

Surprisingly, in the Hassett analysis, small, node negative cancers were associated with a higher odds of chemotherapy use. Surprisingly, node positive and large node negative cancers were associated with a lower chance of chemotherapy use following testing.

Today, the use of this testing is extremely widespread in my community. At each tumor board, patients with stage 1 or 2 breast cancer are nearly universally recommended for such testing. The NCCN clinical practice guidelines suggests using this test to help make the clinical decision regarding the addition of chemotherapy.

However, the intermediate risk group identified in the Oncotype DX testing is still the subject of an ongoing randomized phase III clinical trial. So the application of the test may not be associated with a clear cut answer as to whether or not chemotherapy is useful. Indeed, the frequency of intermediate test results seems to be increasing (Abstracts ASCO 2012). It is important to realize that until such a trial to determine the predictive utility of an intermediate result is completed, the study may be inconclusive. Furthermore, none of the gene expression profile tests have been subjected to a phase III prospective randomized trial (so far only retrospective data has been used).

In my practice, discussing the uncertainty of this testing and applying one of the tests selectively is an important component of breast cancer adjuvant care. Therefore, such patients require several comprehensive visits to both evaluate the appropriateness of possible chemotherapy, and to evaluate the results of testing.

The advance that these tests provide in care of cancer patients must be associated with continued awareness of the results of ongoing randomized prospective trials. The application of similar tests to colorectal cancer, lung cancer and other tumors remains a challenge for clinical trials as well as for the adoption into clinical practice.

gdpawel · 02-09-2013, 02:38 PM

The first prospective trial of the 70-gene-signature MammaPrint (Agendia) breast cancer test shows that it can help determine which breast cancer patients can forgo adjuvant systemic treatment.

The results of the Microarray Prognostics in Breast Cancer (RASTER) study were published online January 31 in the International Journal of Cancer.

Of the women deemed to be low risk by the MammaPrint test, 85% chose not to undergo adjuvant chemotherapy, and 97% were disease-free after 5 years. Of the women deemed to be high risk, 91% underwent chemotherapy were disease-free at 5 years.

It might be prudent to incorporate MammaPrint results with the traditional clinical parameters, but only in patients older than 45 years for whom the value of adjuvant chemotherapy is unclear, said lead author Sabine C. Linn, MD, PhD, from the Department of Medical Oncology at the Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital in Amsterdam.

The RASTER study is the first to prospectively evaluate the performance of MammaPrint. Decisions about adjuvant therapy were made on the basis of the 2004 Dutch Institute of Healthcare Improvement (CBO) guidelines, MammaPrint results, and preferences of clinicians and their patients.

Five-year distant-recurrence-free-interval probabilities estimated with MammaPrint and another clinical common tool, Adjuvant! Online (AOL) — used to assess the risk of developing recurrent disease and/or dying within 10 years — were compared.

Points to Ponder

This study is an important step forward, according to Christopher Benz, MD, who is director of the cancer and developmental therapeutics program at the Buck Institute for Research on Aging in Novato, California. He was not involved in the study.

"The study has largely accomplished its primary aims of demonstrating the feasibility of implementing a multigene signature test in a community-based setting and showing that its implementation can have a significant impact on medical decision-making," he told Medscape Medical News.

In more than 25% of the study population, MammaPrint gave a risk estimate (low risk) that was discordant with the AOL risk estimate (high risk). However, the researchers assumed that clinicians equate a high-risk estimate from AOL with a less than 90% chance of recurrence in 10 years, "a definition that is not necessarily used in common practice," Dr. Benz explained.

On the basis of that definition, 124 of 427 patients in this study were classified as high risk by AOL but low risk by MammaPrint, he continued. Despite this discordance, more than 75% of Dutch clinicians chose not to recommend adjuvant chemotherapy.

"As apparent validation of the MammaPrint prediction, the authors show that over 98% of these patients were still disease-free 5 years later," Dr. Benz noted. Although this makes gene-signature tests like MammaPrint appealing to oncologists "it is hazardous to draw conclusions from breast cancer recurrence rates after only 5 years of follow-up," he said.

In the RASTER study, all breast cancers were node-negative and 80% were estrogen-receptor (ER)-positive. "The natural history of such breast tumors is that most clinical relapses do not occur until 5 or even 10 years after diagnosis — with or without the use of adjuvant therapy," he added.

MammaPrint vs Oncotype

MammaPrint and Oncotype DX (Genomic Health) are the 2 major gene-profiling tests for breast cancer currently available, and there are notable differences between the 2. Oncotype DX measures the expression of 21 genes with polymerase chain reaction, and can use fixed tissue. MammaPrint applies microarray technology to a 70-gene signature, but requires fresh samples.

In addition, MammaPrint can be used in patients with any ER status, whereas Oncotype DX can only be used in ER-positive patients. "MammaPrint is also useful in HER2-positive disease, but Oncotype is not," said Dr. Linn. "There is currently uncertainty about the magnitude of additional information generated by Oncotype DX, since a British group showed that Oncotype is similar to immunohistochemical testing for ER, PGR, HER2, and Ki67," she explained.

But like MammaPrint, Oncotype DX is often discordant with the AOL risk estimator. "Its recurrence score specifically addresses whether an ER-positive breast cancer patient will likely benefit from adjuvant chemotherapy in addition to adjuvant hormonal therapy, whereas the MammaPrint gene signature does not," he said.

American clinicians "are eagerly awaiting the results of the randomized MINDACT trial, which will definitively address the accuracy of this 70-gene signature, relative to AOL, and regardless of tumor ER status," in predicting which breast cancer patients can safely avoid adjuvant chemotherapy, Dr. Benz explained.

Study Details

The primary goal of RASTER was to evaluate MammaPrint in a community-based setting and to study its clinical impact on decision making for adjuvant therapy.

The definitions of high risk and low risk used by Dr. Linn and colleagues were in accordance with CBO guidelines. Patients of low clinical risk were older than 35 years with a grade 1 tumor of 30 mm or smaller, a grade 2 tumor of 20 mm or smaller, or a grade 3 tumor of 10 mm or smaller; or they were younger than 36 years with a grade 1 tumor of 10 mm or smaller.

All other patients were considered to be at high risk.

Adjuvant endocrine treatment in the CBO guidelines is only advised in clinically high-risk patients with hormone-receptor-positive tumors in combination with chemotherapy.

The median follow-up was 61.6 months. In the MammaPrint group, 15% (33 of 219) of the low-risk patients received adjuvant chemotherapy, as did 81% (69 of 208) of the high-risk ones.

The 5-year distant-recurrence-free-interval probabilities in the low-risk and high-risk MammaPrint groups were 97.0% and 91.7%, respectively. The probabilities in the low-risk (n = 132) and high-risk (n = 295) AOL groups were 96.7% and 93.4%, respectively.

The researchers observed that the MammaPrint and AOL risk estimations were discordant in 38% of the cases (161 of 427 patients). Most of these (29%) were low-risk MammaPrint and high-risk AOL; 9% were high-risk MammaPrint and low-risk AOL.

Of the patients who were categorized as low risk on both MammaPrint and AOL, 93% did not receive any adjuvant therapy (not chemotherapy or endocrine therapy). In addition, 56% of patients who were low-risk MammaPrint and high-risk AOL did not receive any adjuvant therapy.

The RASTER study was financially supported the Dutch Health Care Insurance Board. Coauthor L.J. van't Veer, PhD, from the Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital and the Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, reports being a shareholder and being employed by Agendia, which markets MammaPrint, and is named as an inventor on the patent. Coauthor M.J. van de Vijver, MD, PhD, from the Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital, is named as an inventor on the MammaPrint patent. Coauthor W.H. van Harten, MD, PhD, from the Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital, reports being a nonremunerated, nonstakeholding member of the supervisory board of Agendia. Coauthor M. Knauer, from the Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital and the Sisters of Charity Hospital and Cancer Center in Linz, Austria, reports receiving unrestricted educational grants from Agendia.

Int J Cancer. Published online January 31, 2013

Citation: Confirmed: MammaPrint Predicts Treatment in Breast Cancer. Medscape. Feb 08, 2013

http://onlinelibrary.wiley.com/doi/1...108590E8BA2A27 A4.d03t03

http://cancerfocus.org/forum/showthread.php?t=795

http://cancerfocus.org/forum/showthread.php?t=243

'lizbeth · 03-16-2013, 05:02 PM

Bumping this up for new members