Robust Guidelines for the Management of HR+ Her2− EBC: Crucial Value of CanAssist Breast

  SFX Search  Permissions and Reprints Ashok Vaid

We congratulate Parikh et al for putting together this guideline for HR+ Her2− early breast cancer (EBC).[1] As we gather this is a culmination of 2 years work that is bold as well as robust enough to give the correct, unambiguous, and clear-cut guidance to the community oncologists.

They have followed a step-by-step process (modified Delphi) that is both transparent and fair.[2]

Most authors focus on numbers. In the development of guidelines, they sometimes forget that the document will finally be used by the community oncologists who otherwise may not have access to the expertise and mentorship of a senior experienced colleague. While focusing on increasing numbers, many previous publications have lost sight of the rigor required or the level of expertise necessary to be mature enough to guide others in tier two or three cities.[3]

Where breast cancer is concerned, more than any other cancer, the value of a multidisciplinary team cannot be underestimated.[4] Parikh et al took the right first step by conducting a survey including 185 oncologists, of which 65% were senior medical oncologists. This adds to the robustness of the entire methodology used and we appreciate the same.

Parikh et al used a well-established, predefined systematic method (modified Delphi). We have used the same process earlier, published our recommendations, and have received positive feedback regarding their utility.[2] Such guidelines are simple to implement by the community oncologists and the process helps give confidence in the patient party.

In the current age of personalized medicine and precision oncology, our focus is to offer the appropriate treatment to those who will benefit most from it and avoid giving it to those where risk outweighs the potential benefit. It is well established that patients with EBC having a low risk of recurrence do not benefit from chemotherapy. In the past, we have found it difficult to achieve this consistently because the only available tests were those discovered and validated in the Caucasian population of United States and Western Europe.[5] [6] Only a miniscule, if any, patients from India have been included in this or similar Western trials. And we all know that blind application of such markers or scorings in the Indian population is not only inappropriate but can also lead to wrong treatment of patients.[5] [6]

Fortunately, CanAssist Breast is the test that has been prospectively validated in our context; data of this phase 3 trial was presented at ESMO Breast in May 2022.[7]

There is ample evidence that such biomarkers, like CanAssist Breast, need to be given priority when arriving at the treatment plan for individual patients, more so than clinical parameters.[8] [9] In other words, when clinical parameters indicate high risk but biomarker score is in favor of low risk, it is safe to avoid additional unnecessary treatment.

In today's era of next-generation sequencing (NGS), gene-based prognostic and predictive testing is increasingly advocated. However, they have not been able to displace age old protein-based biomarker testing like hormone receptor testing by immunohistochemistry (IHC). This is because these tests have become objective and are time tested over generations. In fact, the more modern NGS tools with higher sensitivity often throw up false negative results or bring to light mutations of unclear significance—the so-called variance of undetermined significance. To this we can add the complexity of the NGS data analytics. While India may have 600 NGS machines among its various laboratories, the turnaround time continues to remain 4 to 6 weeks because of the bioinformatics bottleneck. No wonder, even when the same genetic change can be identified with various techniques, IHC still remains the gold standard, as with ALK (anaplastic lymphoma kinase) mutations seen in lung cancer.[10]

With CanAssist Breast having completed 6 years of real-world clinical utility in India, we look forward to it guiding the treatment decisions among more and more patients with HR+ Her2− EBC, avoiding unnecessary toxicity among low-risk category and ensuring systemic therapy preventing recurrence in the high-risk category.

Publication History

Article published online:
23 August 2022

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