Hormone receptor positive HER2 negative breast cancer – Diagnostics – Overview of Information and Clinical Research

Hormone receptor positive HER2 negative breast cancer represents about 70% of all breast cancer cases. Understanding how this specific type of cancer is diagnosed helps patients and their doctors make informed decisions about treatment. The diagnostic process involves multiple steps, from initial screenings to detailed laboratory tests that examine the unique characteristics of cancer cells.

Introduction: When to Seek Diagnostic Testing

Anyone experiencing unusual changes in their breasts should consider seeking diagnostic testing, regardless of whether those changes seem minor or significant. Not every breast change indicates cancer, but early evaluation remains essential for peace of mind and timely treatment if needed^[1].

Women should look out for specific warning signs that warrant immediate medical attention. These include a new lump or hardened area in or near the breast or armpit that doesn’t change with menstrual cycles, changes in breast size or shape, or skin changes affecting the breast or nipple such as dimpling, puckering, scaling, itching, or unusual discoloration that appears reddish, purple, or darker than normal. Nipple discharge, especially if bloody or clear, and a nipple that pulls inward are also concerning signs^[1].

It’s crucial to understand that breast cancer doesn’t always cause visible or noticeable changes, especially in its early stages. This is precisely why regular breast cancer screenings matter so much. Many benign, or non-cancerous, conditions can cause similar symptoms, making professional evaluation necessary to distinguish between harmless changes and serious concerns^[1].

People with certain risk factors should be particularly vigilant about seeking diagnostic testing. Those who have inherited genetic mutations such as BRCA1 or BRCA2, individuals with a personal or family history of breast cancer, and anyone with long-term exposure to high levels of estrogen or progesterone face elevated risk. This includes people who started menstruating at an early age, experienced menopause late in life, or used certain forms of hormone therapy^[1].

⚠️ Important

Regular breast cancer screenings can detect cancer before symptoms appear. Even without noticeable changes, scheduled mammograms and clinical breast exams help catch cancer at its earliest, most treatable stages. Don’t wait for symptoms to develop before scheduling routine screenings.

Classic Diagnostic Methods

When breast cancer is suspected, doctors use a combination of clinical examinations and advanced imaging to identify the disease and distinguish it from other conditions. The diagnostic journey typically begins with a thorough clinical breast exam, during which a healthcare provider carefully examines the breasts and surrounding areas for any unusual findings^[3].

Imaging tests form the backbone of breast cancer diagnosis. Mammography, which uses low-dose X-rays to create detailed images of breast tissue, remains one of the most important screening and diagnostic tools. When mammograms reveal suspicious areas, doctors may order additional imaging to get a clearer picture. Digital mammography has improved the detection of abnormalities, particularly in women with dense breast tissue^[3].

Ultrasound examinations use sound waves to create images of breast tissue and help doctors determine whether a lump is solid or fluid-filled. This distinction matters because solid masses are more likely to be cancerous, while fluid-filled cysts are typically benign. Ultrasound is particularly useful for examining dense breast tissue and guiding needle biopsies to ensure samples are taken from the correct location^[4].

Magnetic resonance imaging (MRI) provides even more detailed views of breast tissue using powerful magnets and radio waves instead of radiation. MRI scans can detect small tumors that might not appear on mammograms and are particularly valuable for women at high risk of breast cancer or those with dense breast tissue. However, MRI is not used as a routine screening tool for everyone due to its higher cost and the potential for false-positive results^[4].

When imaging reveals suspicious areas, a tissue biopsy becomes necessary. During a biopsy, doctors remove a small sample of tissue from the suspicious area for examination under a microscope. Several types of biopsies exist, ranging from fine needle aspiration, which uses a thin needle to extract cells, to core needle biopsy, which removes a larger tissue sample using a hollow needle. In some cases, surgical biopsy may be necessary to remove the entire suspicious area^[3].

After obtaining tissue samples, pathological evaluation provides the definitive diagnosis. Pathologists, who are doctors specializing in disease diagnosis through tissue examination, analyze the biopsy samples under microscopes. They look at the appearance and behavior of cells to determine whether cancer is present and, if so, what type of cancer it is^[2].

The pathological evaluation includes crucial tests to determine the cancer’s characteristics, or biomarkers. For hormone receptor positive HER2 negative breast cancer specifically, pathologists test whether cancer cells have receptors for estrogen and progesterone. These receptors are proteins on the cell surface that hormones can attach to. When breast cancer cells have these receptors, the cancer is called hormone receptor positive. Specifically, cancers with estrogen receptors are called ER-positive, while those with progesterone receptors are called PR-positive^[7].

Breast cancers are considered ER-positive when at least 1% of cells test positive for estrogen receptors. The same threshold applies to PR-positive cancers. Many cancers are positive for both receptors, though some may be positive for only one. Doctors have identified a category called ER Low Positive tumors, which have low levels of ER positivity between 1% and 10%, and these tend to behave more like hormone receptor negative tumors^[3].

Pathologists also test for HER2, which stands for human epidermal growth factor receptor 2. This protein appears on the surface of some breast cancer cells and promotes their growth. The test determines whether cancer cells have excess amounts of HER2 protein or extra copies of the HER2 gene. When cancer cells don’t have high levels of HER2, the cancer is classified as HER2-negative^[1].

Testing for hormone receptors typically uses a method called immunohistochemistry (IHC), which measures how many hormone receptors are present on cancer cells. The results come back as a percentage, with higher percentages meaning the tumor is more responsive to hormones. This information proves vital because it determines which treatments are likely to work best^[4].

Clinical staging represents another critical component of diagnosis. Doctors document the tumor size, lymph node involvement, and whether cancer has spread to other parts of the body using a combination of clinical and radiological examinations. This staging system helps doctors understand how advanced the cancer is and guides treatment decisions^[3].

⚠️ Important

If breast cancer returns or spreads to other parts of the body, your hormone receptor status can change. Cancer that has been treated with hormone therapies may become resistant to those same treatments, or tumors may undergo genetic changes. This is why doctors may recommend retesting the cancer’s biomarkers if it comes back or progresses, ensuring treatment remains appropriately targeted^[4].

Diagnostics for Clinical Trial Qualification

Clinical trials investigating new treatments for hormone receptor positive HER2 negative breast cancer use specific diagnostic criteria to determine which patients can participate. These qualification tests go beyond standard diagnostic procedures to include specialized biomarker testing and genetic analyses that help researchers match patients to the most appropriate experimental treatments^[14].

Standard pathological assessment remains the foundation for clinical trial enrollment. Researchers require confirmation that cancer cells are indeed hormone receptor positive and HER2 negative according to established criteria. This means documented evidence that at least 1% of cancer cells express estrogen or progesterone receptors, and that HER2 testing shows negative results through either immunohistochemistry or another validated testing method^[3].

Genomic assays have become increasingly important for clinical trial qualification in recent years. These sophisticated laboratory tests examine multiple genes within tumor samples to provide information about how likely the cancer is to grow and spread, and how it might respond to specific treatments. Several commercially available genomic tests exist, and many clinical trials now include these assessments as part of their enrollment criteria^[3].

Next-generation sequencing represents an advanced diagnostic tool that analyzes multiple genes simultaneously. This technology allows researchers to identify specific genetic mutations or alterations within tumors that might respond to targeted therapies being tested in clinical trials. For hormone receptor positive HER2 negative breast cancer, next-generation sequencing can reveal mutations in genes such as PIK3CA or BRCA, which may make patients eligible for trials testing drugs that target these specific alterations^[14].

Some clinical trials specifically seek patients with BRCA gene mutations. These inherited genetic changes increase breast cancer risk overall, and cancers in people with BRCA mutations may respond differently to certain treatments. Testing for BRCA mutations typically involves a blood test rather than tumor tissue analysis, since these mutations are present in all cells of the body, not just cancer cells^[14].

The PIK3CA gene mutation occurs specifically within tumor cells and appears in a significant portion of hormone receptor positive HER2 negative breast cancers. Trials testing medications that target this mutation require proof through tumor tissue testing that the mutation is present. This type of targeted testing has become standard practice when considering enrollment in trials investigating PIK3CA-specific therapies^[14].

Clinical trials often have strict requirements regarding the stage of disease at diagnosis. Some trials accept only patients with early-stage disease who have not yet received treatment, while others specifically recruit patients with metastatic cancer that has spread beyond the breast and nearby lymph nodes to other organs. Confirmation of disease stage through appropriate imaging and clinical assessment remains essential for trial qualification^[3].

Many trials require fresh tissue biopsies before enrollment, even in patients who already have a confirmed diagnosis. This ensures that researchers have adequate tissue samples for all planned biomarker analyses and helps verify that the cancer’s characteristics haven’t changed since the original diagnosis. These research biopsies follow the same procedures as diagnostic biopsies but may collect additional tissue for experimental testing^[4].

Blood-based biomarker testing is increasingly common in clinical trial protocols. Researchers may measure levels of certain proteins or genetic material circulating in the bloodstream that provide information about cancer activity. These blood tests, sometimes called liquid biopsies, can supplement tissue-based testing and may be repeated throughout the trial to monitor how cancer responds to treatment^[14].

Performance status assessment represents another qualification criterion for most clinical trials. Doctors evaluate how well patients can carry out normal daily activities and whether they have sufficient physical reserves to tolerate experimental treatments. This assessment doesn’t involve laboratory tests but rather clinical evaluation of overall health and functionality^[3].

Some trials investigating combination treatments require testing to ensure adequate organ function before enrollment. This typically includes blood tests to check kidney and liver function, heart function tests such as echocardiograms, and sometimes bone marrow function assessment through blood cell counts. These tests protect patient safety by identifying individuals who might experience severe complications from experimental treatments^[3].

Prognosis and Survival Rate

Prognosis

The outlook for people with hormone receptor positive HER2 negative breast cancer depends on multiple factors that doctors consider when discussing individual prognoses. Hormone receptor positive HER2 negative cancers generally grow more slowly than hormone receptor negative cancers, which often translates to better long-term outcomes^[4].

The stage at which cancer is diagnosed significantly influences prognosis. Most patients receive their diagnosis at an early stage, when cancer remains confined to the breast or nearby lymph nodes. Early detection through screening programs has contributed to improved survival outcomes in recent years. The vast majority of breast cancers are diagnosed at an early stage, providing more treatment options and generally better chances of long-term survival^[3].

Individual tumor characteristics beyond just hormone receptor and HER2 status affect prognosis. Factors such as tumor size, lymph node involvement, how abnormal the cancer cells look under a microscope, and how fast the cancer cells are dividing all play roles in determining likely outcomes. Doctors consider all these elements together rather than in isolation when discussing prognosis with patients^[3].

Expression levels of hormone receptors also matter for prognosis. Cancers with higher percentages of cells expressing estrogen or progesterone receptors typically respond better to hormone-based treatments. However, newly defined ER Low Positive tumors, which have between 1% and 10% of cells expressing estrogen receptors, tend to behave more like hormone receptor negative tumors and may have different outcomes compared to cancers with higher receptor expression^[3].

The balance between estrogen and progesterone receptor expression influences outcomes as well. Research has shown that unbalanced hormone receptor expression, such as being positive for only one receptor type, may result in different survival rates compared to cancers positive for both receptors. Patients whose cancers express both estrogen and progesterone receptors generally have better responses to treatment and improved long-term survival^[5].

Survival rate

Hormone receptor positive HER2 negative breast cancer has among the most favorable survival statistics of all breast cancer types, particularly when diagnosed early. Because this represents the most common subtype, accounting for approximately 70% of all breast cancers, substantial research has focused on improving outcomes for these patients^[1].

Significant advances in treatment over recent years have resulted in improved survival outcomes for people with early-stage hormone receptor positive HER2 negative breast cancer. The development of effective hormone therapies, improvements in surgical techniques, and better understanding of which patients benefit from additional treatments beyond hormone therapy have all contributed to better survival rates^[3].

For metastatic hormone receptor positive HER2 negative breast cancer, where cancer has spread to distant organs, treatment focuses on controlling the disease and maintaining quality of life rather than cure. Nearly 30,000 patients die from this disease each year in the United States, though marked changes in treatment over the past five years have improved outcomes. The introduction of new drug classes that can be combined with hormone therapy has transformed the approach to metastatic disease^[6].

Individual survival rates vary considerably based on the specific characteristics mentioned in the prognosis section above. Two patients with the same breast cancer subtype may have different outcomes depending on factors like tumor size at diagnosis, lymph node involvement, overall health status, and how well their particular cancer responds to treatment. This variability underscores why personalized treatment planning based on individual tumor characteristics remains so important^[3].

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