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PIK3CA-activated mutation – Diagnostics

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Diagnosing PIK3CA-activated mutation involves testing cancer tissue or blood samples to identify specific genetic changes that can drive tumor growth and influence treatment decisions, with different testing methods available to detect these mutations and guide personalized therapy approaches.

Introduction

Understanding whether you or a loved one should undergo diagnostic testing for PIK3CA mutations is an important step in managing certain types of cancer. PIK3CA is a gene that provides instructions for making a protein called p110 alpha, which plays a key role in controlling how cells grow, divide, and survive. When this gene develops mutations, cells can grow uncontrollably, potentially leading to cancer.[1]

Anyone diagnosed with cancer, particularly breast cancer, colorectal cancer, bladder cancer, or certain other solid tumors, may benefit from PIK3CA mutation testing. These mutations are found in approximately 30 to 40 percent of breast cancers and are also present in 20 to 25 percent of colon cancers and 10 percent of rectal cancers.[4][5] The mutations are not inherited from parents but develop during a person’s lifetime, appearing only in the tumor cells themselves.[1]

Testing becomes particularly important when making treatment decisions for advanced or metastatic cancer. For example, patients with hormone receptor-positive, HER2-negative breast cancer who have advanced disease should consider PIK3CA testing, as the results can determine whether specific targeted therapies will be effective.[13] The presence of certain PIK3CA mutations may mean that a tumor responds differently to various treatments, and knowing your mutation status helps doctors personalize your care plan.

You should discuss PIK3CA testing with your oncologist when you receive an initial cancer diagnosis, especially if the cancer has spread beyond its original location. Testing may also be recommended if your cancer progresses during treatment or if you are considering participating in a clinical trial. Early testing allows for more treatment options and helps avoid delays in starting the most appropriate therapy for your specific cancer type.

⚠️ Important
PIK3CA mutations are not hereditary and do not pass from parents to children. They are somatic mutations, meaning they occur only in tumor cells during a person’s lifetime. Family members do not need to be tested based on your PIK3CA mutation status, as these changes affect only cancer cells and are not present throughout your body.

Diagnostic Methods

Several testing approaches are available to identify PIK3CA mutations in cancer cells. The choice of method depends on the type of cancer, the stage of disease, and what tissue samples are available for testing. Each method has specific strengths and can detect different types of genetic changes in the PIK3CA gene.

Tissue Biopsy Testing

The most common way to test for PIK3CA mutations involves analyzing a sample of tumor tissue obtained through a biopsy. During this procedure, a doctor removes a small piece of cancerous tissue, which is then sent to a specialized laboratory for genetic analysis. The biopsy sample can come from the primary tumor or from areas where the cancer has spread.[4]

Tissue testing is considered the gold standard because it directly examines the cancer cells themselves. For breast cancer patients, the tissue sample typically comes from either the original breast tumor removed during surgery or from a biopsy of a metastatic site. In colorectal cancer, tissue samples are usually obtained during colonoscopy or from surgical specimens.[4] It’s worth noting that mutation status doesn’t always match between the primary tumor and metastatic sites, which is why doctors sometimes test both locations to get the most accurate picture.

Blood-Based Testing (Liquid Biopsy)

A newer approach involves testing blood samples for PIK3CA mutations, often called liquid biopsy or circulating tumor DNA (ctDNA) testing. When cancer cells die, they release small fragments of DNA into the bloodstream. Laboratory techniques can detect and analyze these DNA fragments to identify mutations without needing to perform an invasive tissue biopsy.[5][11]

Blood testing offers several advantages: it’s less invasive than tissue biopsy, can be repeated more easily to monitor changes over time, and may detect mutations from multiple tumor sites at once. For patients with breast cancer, blood samples are drawn from the arm just like any routine blood test. The FDA has approved blood-based PIK3CA testing methods for certain cancer types, and this approach is particularly useful when tissue samples are difficult to obtain or when monitoring treatment response.[5]

However, if a blood test returns a negative result (no mutation detected), doctors often recommend confirming with tissue testing. This is because blood tests may miss mutations when tumor DNA levels in the blood are very low, leading to false-negative results where the mutation is actually present but not detected.[11]

Next-Generation Sequencing

Next-generation sequencing (NGS) is a comprehensive testing method that can examine multiple genes simultaneously, including PIK3CA and many other cancer-related genes. This technology reads the DNA sequence of cancer cells and identifies any mutations present. NGS panels can detect a wide variety of PIK3CA mutations throughout the entire gene, not just the most common ones.[4][13]

NGS testing is particularly valuable because PIK3CA mutations can occur at many different locations within the gene. While certain “hotspot” mutations are more common—such as those in exon 9 and exon 20 of the gene—less common mutations also exist and may have different effects on how cancer behaves and responds to treatment.[5] An exon is a segment of a gene that contains instructions for making proteins. The majority of PIK3CA mutations, approximately 80 percent, occur in exon 9 and exon 20, but NGS can detect mutations throughout all 20 exons of the gene.[4]

NGS testing typically takes one to two weeks to complete once the laboratory receives the sample. The comprehensive nature of NGS means that in addition to PIK3CA, doctors can learn about other genetic changes in the tumor that might influence treatment decisions or clinical trial eligibility.

Targeted Mutation Panels

Some diagnostic tests focus specifically on detecting the most common PIK3CA mutations rather than sequencing the entire gene. The therascreen PIK3CA test, for example, is an FDA-approved companion diagnostic that detects 11 specific hotspot mutations in the PIK3CA gene.[5][10] These targeted panels use techniques like polymerase chain reaction (PCR), which amplifies specific DNA sequences to make mutations easier to detect.

The advantage of targeted panels is that they provide rapid, accurate results for the mutations they’re designed to detect. However, they have an important limitation: they only identify specific predetermined mutations. Research shows that the therascreen panel would identify about 72 percent of all PIK3CA mutations and correctly classify about 80 percent of patients with PIK3CA-mutated breast cancer.[5] This means approximately 20 percent of patients with a PIK3CA mutation might receive a negative result on this test because their specific mutation isn’t included in the panel.

Understanding Mutation Hotspots

PIK3CA mutations are not randomly distributed throughout the gene. Most occur at specific locations called hotspots, particularly affecting certain amino acids in the p110 alpha protein. The five most common mutations account for about 73 percent of all PIK3CA mutations in breast cancer: H1047R (35 percent), E545K (17 percent), E542K (11 percent), N345K (6 percent), and H1047L (4 percent).[5]

Understanding these patterns matters because different mutations may have different effects. Mutations in exon 9, such as E542K and E545K, affect what’s called the helical domain of the protein. Mutations in exon 20, such as H1047R, affect the kinase domain, which is the part of the protein that performs the actual biochemical work.[7] Some research suggests that mutations in different domains may lead to different clinical outcomes, though this remains an area of active investigation.

About 12 percent of patients with PIK3CA-mutated tumors actually have two different PIK3CA mutations in the same tumor, called double mutations. These cases can be particularly challenging to detect with targeted mutation panels, as the panels may identify only one of the two mutations or miss both if neither is included in the test.[5]

Diagnostics for Clinical Trial Qualification

When patients are being considered for clinical trials testing new treatments for PIK3CA-mutated cancers, specific diagnostic requirements must be met. Clinical trials have strict inclusion criteria—the requirements patients must meet to participate—and PIK3CA mutation testing is often a key component of determining eligibility.

Standard Testing Requirements

Most clinical trials evaluating treatments that target PIK3CA mutations require confirmed mutation status before enrollment. This confirmation typically must come from a certified laboratory using a validated testing method. The trial protocol will specify exactly which testing method is acceptable, which mutations qualify for enrollment, and how recent the test must be.[9]

For many trials, mutation testing must be performed on tumor tissue obtained within a certain timeframe, often within the past year. This requirement exists because tumors can change over time, and the mutation profile of a cancer at diagnosis may differ from the profile after treatment. Some trials accept blood-based testing results, while others require tissue confirmation regardless of blood test results.

Specific Mutation Requirements

Not all clinical trials accept all PIK3CA mutations. Some trials focus specifically on the most common hotspot mutations in exon 9 or exon 20, while others may be designed to test treatments for any activating PIK3CA mutation. The trial informed consent document will clearly state which specific mutations qualify for participation.[9]

Understanding this distinction is crucial because a patient might have a PIK3CA mutation but not be eligible for a particular trial if their specific mutation isn’t included in the trial’s criteria. For example, a trial testing a treatment designed specifically for H1047R mutations would not accept patients with E545K mutations, even though both are common PIK3CA mutations.

Testing Timing and Documentation

Clinical trials typically require official documentation of mutation status from an accredited laboratory. A report from the testing laboratory must include specific information: the testing method used, the exact mutation identified (using standard nomenclature), the percentage of tumor cells carrying the mutation (called variant allele frequency), and confirmation that the test was performed according to validated procedures.

If your original diagnostic testing didn’t use a method acceptable to a specific trial, you may need to have additional testing performed. Your oncologist and the trial coordinator can help determine whether retesting is necessary and arrange for appropriate samples to be sent to a qualified laboratory. This process can take several weeks, so it’s important to start discussions about clinical trial participation early.

⚠️ Important
If you’re interested in clinical trials, discuss PIK3CA testing with your doctor at the time of diagnosis or when your cancer progresses. Having comprehensive mutation testing early, preferably using next-generation sequencing, can open more trial opportunities and avoid delays. Some trials fill quickly, and having your mutation status documented in advance helps you move through the enrollment process more efficiently.

Re-testing for Clinical Trials

In some situations, clinical trials may require fresh biopsy samples rather than using archived tissue from an earlier diagnosis. This requirement ensures that the mutation profile reflects the current state of the cancer, especially if the cancer has been treated or if significant time has passed since the original diagnosis. Advanced cancers can acquire additional mutations over time or after treatment, and these changes might affect how the cancer responds to experimental therapies.

Re-biopsy procedures are typically performed when clinically feasible and safe. Your medical team will evaluate whether the potential benefits of clinical trial participation justify the risks and discomfort of an additional biopsy. In cases where re-biopsy isn’t possible due to tumor location or patient health considerations, trials may accept previous testing results or allow blood-based testing as an alternative.

Companion Diagnostic Requirements

Some clinical trials use companion diagnostics—specific FDA-approved tests designed to identify patients who will benefit from a particular treatment. When a trial requires a companion diagnostic, you must be tested using that exact test, even if you’ve had other PIK3CA testing. The therascreen PIK3CA test serves as a companion diagnostic for the drug alpelisib in breast cancer treatment.[5][10]

Companion diagnostics undergo rigorous validation to ensure they accurately identify patients who should receive the associated treatment. Using the required companion diagnostic gives both you and your doctors confidence that the treatment is appropriate for your specific cancer. Insurance coverage for these tests is often better when they’re performed as part of clinical care or trial enrollment.

Prognosis and Survival Rate

Prognosis

The presence of PIK3CA mutations in cancer appears to have complex effects on prognosis that vary depending on cancer type, the specific mutation present, and other characteristics of the tumor. Research examining 2,587 patients with breast cancer found that patients whose tumors harbor PIK3CA mutations actually have a better clinical outcome compared to those with wild-type PIK3CA (no mutation). This improved prognosis appears to be particularly relevant for postmenopausal women with estrogen receptor-positive breast cancer and may be most pronounced in patients with mutations specifically in the kinase domain of the p110 alpha protein.[12]

This finding is somewhat surprising because PIK3CA mutations cause increased cell growth and division, which typically suggests more aggressive cancer behavior. Several explanations have been proposed for this paradox. PIK3CA mutations may interfere with the cancer’s ability to spread to distant sites (metastasize) or may trigger cellular aging processes called senescence, which slows tumor growth. Another possibility is that PIK3CA mutations may make breast tumors more detectable at earlier stages by altering the structure of cancer cells, leading to earlier diagnosis when treatment is most effective. Additionally, PIK3CA mutations may predict favorable response to hormonal therapy in hormone receptor-positive breast cancer, giving these patients a therapeutic advantage.[12][15]

However, the location of the mutation within the PIK3CA gene matters. In colorectal cancer, mutations in exon 20 of PIK3CA are associated with less favorable responses to certain treatments, specifically EGFR inhibitor therapy. Colorectal cancers with PIK3CA exon 20 mutations show reduced responsiveness to these targeted therapies compared to tumors without these mutations.[4] This demonstrates that the clinical impact of PIK3CA mutations is not uniform across all cancer types or all mutation types.

The relationship between PIK3CA mutations and treatment outcomes continues to be investigated through ongoing clinical trials. What is becoming clear is that PIK3CA mutation status provides valuable prognostic information that should be considered alongside other tumor characteristics when estimating disease course and planning treatment approaches.

Survival Rate

Specific survival rate statistics for PIK3CA-mutated cancers are challenging to define because outcomes vary significantly based on cancer type, stage at diagnosis, specific mutation, and treatments received. The available evidence suggests that in breast cancer, the presence of PIK3CA mutations is generally associated with favorable survival outcomes when compared to PIK3CA wild-type tumors, particularly in hormone receptor-positive disease.[12]

Analysis of large patient cohorts has shown that breast cancer patients with PIK3CA mutations may experience better overall survival and disease-free survival compared to those without mutations. This survival advantage appears most consistent when the mutation occurs in specific domains of the protein and when the cancer is hormone receptor-positive and HER2-negative.[15] However, survival outcomes are influenced by many factors beyond mutation status, including tumor stage, grade, response to treatment, and the patient’s overall health.

It’s important to recognize that survival statistics represent averages across large groups of patients and may not predict any individual patient’s outcome. Advances in targeted therapies specifically designed for PIK3CA-mutated cancers, such as alpelisib for breast cancer, are changing the landscape of treatment and potentially improving outcomes for these patients. As these newer treatments become more widely used and more data is collected, our understanding of survival rates in PIK3CA-mutated cancers will continue to evolve.

Ongoing Clinical Trials on PIK3CA-activated mutation

  • Study of RLY-2608 for Adults and Children with PIK3CA-Related Overgrowth and Malformations

    Recruiting

    1 1
    Investigated diseases:
    Investigated drugs:
    Belgium France Germany Ireland Italy Norway +1

  • Study on Alpelisib and Fulvestrant for Advanced Breast Cancer in Patients with PIK3CA Mutation and Hormone-Receptor Positive, HER2 Negative Tumors

    Not recruiting

    1 1 1
    Investigated diseases:
    Investigated drugs:
    The Netherlands

References

https://medlineplus.gov/genetics/gene/pik3ca/

https://pmc.ncbi.nlm.nih.gov/articles/PMC3781181/

https://www.nature.com/articles/s41467-023-35789-6

https://www.knowyourbiomarker.org/biomarkers/pik3ca

https://breast-cancer-research.biomedcentral.com/articles/10.1186/s13058-020-01284-9

https://pmc.ncbi.nlm.nih.gov/articles/PMC3164550/

https://pmc.ncbi.nlm.nih.gov/articles/PMC11944057/

https://ecancer.org/en/news/26071-new-advances-in-targeted-therapies-for-pik3ca-mutated-cancers

https://pmc.ncbi.nlm.nih.gov/articles/PMC3072168/

https://breast-cancer-research.biomedcentral.com/articles/10.1186/s13058-020-01284-9

https://massivebio.com/pik3ca-gene-ultimate-guide/

https://pmc.ncbi.nlm.nih.gov/articles/PMC3777497/

https://www.azprecisionmed.com/breast-cancer/pik3ca-akt1-pten-mutations

https://www.knowyourbiomarker.org/biomarkers/pik3ca

https://pmc.ncbi.nlm.nih.gov/articles/PMC4054885/

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PIK3CA-activated mutation:

FAQ

What does it mean if my PIK3CA test result is negative?

A negative result means that the testing method used did not detect any PIK3CA mutations in your sample. This is reported as “PIK3CA wild-type” or “PIK3CA WT.” However, it’s important to understand that no test is perfect. If the test was blood-based, your doctor might recommend confirming with tissue testing, as blood tests can sometimes miss mutations when tumor DNA levels are low. Additionally, if a targeted mutation panel was used rather than comprehensive sequencing, you might have a rare PIK3CA mutation that wasn’t included in the panel being tested.[4][11]

Will my insurance cover PIK3CA mutation testing?

Insurance coverage for PIK3CA testing varies by provider and situation. Many insurance companies cover this testing when it’s ordered by your oncologist for cancer diagnosis or treatment planning, particularly for breast cancer and colorectal cancer. FDA-approved tests like the therascreen PIK3CA test often have better insurance coverage, especially when the results will directly influence treatment decisions, such as whether to use alpelisib for breast cancer. Your doctor’s office or the testing laboratory can usually verify your coverage before performing the test. Some laboratories also offer financial assistance programs for patients with limited insurance coverage.[5]

How long does it take to get PIK3CA test results?

The turnaround time depends on the testing method and laboratory. Targeted mutation panels using PCR technology may provide results in as little as a few days to one week. Next-generation sequencing typically takes one to two weeks from the time the laboratory receives your sample. Blood-based testing may be slightly faster than tissue testing in some cases. Keep in mind that additional time is needed for your doctor to receive, review, and discuss the results with you. If you’re waiting for results to make treatment decisions or enroll in a clinical trial, ask your healthcare team about the expected timeline when the test is ordered.[4]

Do I need to be retested if my cancer comes back or spreads?

This depends on your specific situation, but retesting is often valuable when cancer recurs or metastasizes. Tumors can change over time and after treatment, potentially acquiring new mutations or losing previous ones. The PIK3CA mutation status doesn’t always match between the primary tumor and metastatic sites, so testing both can provide important information. Additionally, if your original testing was done with a limited panel and new treatment options have become available, comprehensive retesting with next-generation sequencing might reveal additional actionable mutations. Your oncologist can help determine whether retesting would be beneficial in your case.[4][9]

If I have a PIK3CA mutation, does that mean targeted therapy will definitely work for me?

Having a PIK3CA mutation means you may be eligible for targeted therapies designed to block the effects of the mutation, but it doesn’t guarantee that these treatments will work. Clinical trials have shown that targeted PIK3CA inhibitors like alpelisib can be effective in many patients with PIK3CA-mutated cancers, but not everyone responds, and the degree of benefit varies. The effectiveness depends on many factors, including the specific mutation you have, what other genetic changes are present in your tumor, the type and stage of your cancer, and previous treatments you’ve received. Your oncologist can discuss the likelihood of benefit from targeted therapy based on your complete clinical picture.[5][9]

🎯 Key takeaways

  • PIK3CA mutations are among the most common genetic changes in cancer, found in 30-40% of breast cancers and 20-25% of colon cancers, making testing highly relevant for many patients
  • Testing can be done using tumor tissue biopsies or blood samples, with each method having specific advantages depending on your situation
  • Next-generation sequencing detects more mutations than targeted panels but takes longer; understanding which test you’re getting matters for accurate results
  • About 20% of PIK3CA mutations might be missed by common diagnostic panels, so comprehensive testing may be worth discussing with your doctor
  • Paradoxically, having a PIK3CA mutation in breast cancer is often associated with better prognosis, especially in hormone receptor-positive disease
  • Clinical trials often have specific mutation requirements, so knowing your exact PIK3CA mutation status can open doors to experimental treatments
  • PIK3CA mutations are not hereditary and don’t affect your family members, as they occur only in cancer cells, not throughout your body
  • Retesting when cancer progresses or spreads can be valuable because tumors change over time and may acquire new mutations or lose old ones

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