Primitive neuroectodermal tumour – Diagnostics – Overview of Information and Clinical Research

Primitive neuroectodermal tumors are rare, aggressive brain tumors that require careful diagnostic evaluation. Understanding when to seek testing and what diagnostic procedures are involved is essential for patients and families navigating this challenging diagnosis.

Introduction: Who Should Undergo Diagnostics and When

Primitive neuroectodermal tumors, often abbreviated as PNET, are a group of rare brain tumors that primarily affect children and young adults. These tumors develop from primitive nerve cells, which are immature cells left over from the early development of the nervous system before a person is born.^[1] When these cells fail to develop normally, they can form tumors that grow quickly and spread easily.

Anyone experiencing persistent or concerning neurological symptoms should consider seeking medical evaluation. The symptoms that suggest a need for diagnostic testing depend largely on where the tumor is located in the brain or spinal cord. Parents should be especially watchful with children who develop unusual patterns of headaches, particularly those that occur in the morning or are accompanied by vomiting.^[3] These morning headaches often improve after vomiting, which is a distinctive pattern that differs from typical headaches.

Other warning signs that warrant prompt medical attention include seizures that appear for the first time, especially in children who have no history of epilepsy. Changes in personality or behavior can also signal a problem, as can unexplained weakness on one side of the body. Parents might notice their child has become unusually sleepy, irritable, or has lost interest in activities they previously enjoyed.^[6] These changes may develop gradually or appear suddenly, but any persistent neurological symptom deserves medical evaluation.

Problems with coordination and balance represent another important category of symptoms. Children or adults might begin having trouble walking, experience dizziness, or develop double vision. Some people experience numbness or tingling sensations, while others have unexplained weight changes either gaining or losing weight without trying.^[1] When tumors develop in the spinal cord rather than the brain, symptoms can include bowel or bladder control problems and pain radiating down the back and legs.

⚠️ Important

Because primitive neuroectodermal tumors are aggressive and fast-growing, early diagnosis is crucial. If you or your child experiences persistent neurological symptoms, especially morning headaches with vomiting, new seizures, or balance problems, seek medical evaluation promptly. These tumors can spread quickly through the fluid surrounding the brain and spinal cord, making timely diagnosis important for treatment planning.

Diagnostic Methods for Identifying PNETs

The diagnostic process for primitive neuroectodermal tumors begins with a thorough physical examination and detailed medical history. Doctors will ask about the timeline of symptoms, their severity, and any patterns that have emerged. This initial consultation helps doctors determine which diagnostic tests are most appropriate.^[9]

A neurological examination is a fundamental first step in evaluating suspected brain or spinal cord tumors. During this exam, the doctor assesses multiple aspects of nervous system function. They test how well the eyes move, checking for problems with coordination between the two eyes that might cause double vision. The doctor evaluates hearing and the sense of smell, both of which can be affected by brain tumors. Muscle strength is tested in the arms and legs, along with reflexes that can reveal problems with nerve pathways.^[6] The examination also includes tests of coordination and balance, such as asking the patient to walk in a straight line or touch their nose with their finger while their eyes are closed.

Magnetic resonance imaging, commonly called an MRI scan, is the primary and most important imaging test for diagnosing primitive neuroectodermal tumors. This sophisticated imaging technique uses powerful magnets and radio waves to create detailed pictures of the brain and spinal cord. Unlike X-rays or CT scans, MRI does not use radiation, making it particularly suitable for children who may need multiple scans over time.^[12]

On an MRI scan, primitive neuroectodermal tumors typically appear as a single mass, most commonly in the cortex, which is the outer layer of the brain. The tumor often shows up brightly on the scan after a contrast agent is injected into a vein. This contrast material, containing substances like gadolinium, helps the tumor stand out more clearly against the normal brain tissue in the background. Sometimes doctors can see fluid-filled pockets called cysts within the tumor mass, and there may be swelling in the brain tissue surrounding the tumor.^[1]

Because these tumors are known to spread through cerebrospinal fluid the clear liquid that bathes the brain and spinal cord it is essential to obtain MRI images of both the brain and the entire spine. This comprehensive imaging approach helps doctors determine if the tumor has spread to other areas of the central nervous system, which affects treatment planning and prognosis.^[3] In some cases, more than one tumor may be visible on the initial MRI, indicating that the disease has already spread.

Computed tomography scans, or CT scans, may also be used in the diagnostic process. CT scans use X-rays taken from multiple angles and processed by a computer to create cross-sectional images of the body. While MRI provides better detail of soft tissues like the brain, CT scans are faster to perform and may be preferred in emergency situations. Like MRI, CT scans often use a contrast agent injected into a vein to help visualize the tumor more clearly.^[9]

The definitive diagnosis of a primitive neuroectodermal tumor requires examination of the actual tumor tissue. This means that a biopsy must be performed, where a sample of the tumor is removed and examined under a microscope. In many cases, this biopsy is performed during the initial surgery to remove as much of the tumor as possible. During the procedure, a neurosurgeon removes a portion of the skull to access the brain, then uses specialized instruments to obtain tumor tissue.^[9]

The tumor sample is sent to a neuropathologist, a doctor who specializes in diagnosing diseases of the nervous system. The neuropathologist examines thin slices of the tumor tissue under a microscope, looking for specific features that identify it as a primitive neuroectodermal tumor. These features include the presence of small, round, undeveloped cells and sometimes distinctive patterns called rosettes, where cells arrange themselves in a circular formation around a central point.^[18]

Additional laboratory tests on the tumor tissue help confirm the diagnosis and classify the specific type of tumor. Immunohistochemical testing identifies specific proteins on the tumor cells. For primitive neuroectodermal tumors, pathologists look for a marker called CD99, which is present in the vast majority of these tumors. They also test for at least two neural markers proteins that indicate the tumor developed from nerve tissue to make an accurate diagnosis.^[18]

Modern diagnostic techniques now include molecular analysis of tumor tissue, examining the genetic characteristics of the tumor cells. In 2016, the World Health Organization revised how these tumors are classified, moving away from grouping them all under the term “PNET” and instead classifying them based on specific genetic features. For example, doctors now look for an amplification of a genetic region called C19MC on chromosome 19. Tumors with this genetic change are classified as embryonal tumor with multilayered rosettes, C19MC-altered, while those without it receive different classifications.^[4]

All primitive neuroectodermal tumors are classified as grade 4 tumors, which is the highest grade on the scale used to classify brain tumors. Grade 4 means these tumors are malignant (cancerous) and fast-growing, with a tendency to spread to other areas. This high grade reflects the aggressive nature of these tumors and helps guide treatment decisions.^[1]

In rare cases, a primitive neuroectodermal tumor may be detected before a child is born through prenatal ultrasound imaging. When this happens, additional imaging and planning can occur before delivery to ensure the medical team is prepared to begin evaluation and treatment as soon as possible after birth.^[9]

Diagnostics for Clinical Trial Qualification

Clinical trials research studies that test new treatments require specific diagnostic criteria to determine which patients are eligible to participate. These criteria ensure that the trial studies a specific group of patients and that the results can be interpreted accurately. For primitive neuroectodermal tumors, the diagnostic requirements for clinical trial enrollment typically mirror the standard diagnostic procedures but may include additional specific tests or criteria.

Complete MRI imaging of both the brain and spine is typically required before enrollment in a clinical trial. This baseline imaging establishes the size and extent of the tumor before any treatment begins, providing a reference point for measuring whether the treatment is effective. The MRI must clearly document the location of all tumor masses and any spread of disease through the cerebrospinal fluid.^[3]

Tissue diagnosis by a neuropathologist is mandatory for clinical trial participation. The tumor must be confirmed as a primitive neuroectodermal tumor or one of the related embryonal tumor types through microscopic examination and molecular testing. Many trials now require specific genetic testing to determine the molecular subtype of the tumor. This genetic information helps match patients to trials testing treatments that target specific molecular features of their tumor.^[4]

Assessment of whether the tumor has spread is crucial for trial eligibility. Doctors need to document whether the tumor is localized to one area or has spread to other parts of the central nervous system or beyond. About one-third of patients have tumors that have already spread at the time of diagnosis. Clinical trials often have specific criteria regarding disease spread, with some trials accepting only patients with localized disease while others focus on patients with more advanced spread.^[1]

Additional blood tests and organ function tests are typically required before clinical trial enrollment. These tests assess the patient’s overall health and ensure they can safely tolerate the experimental treatment being studied. Blood counts must be adequate, and the liver and kidneys must be functioning well enough to process medications. Heart function may also be evaluated, particularly if the trial involves chemotherapy drugs that can affect the heart.

Some clinical trials require testing of cerebrospinal fluid to look for tumor cells. This involves a procedure called a lumbar puncture or spinal tap, where a thin needle is inserted between the vertebrae in the lower back to collect a small sample of the fluid surrounding the spinal cord. A pathologist examines this fluid under a microscope to determine if tumor cells are present, which provides information about whether the tumor has spread through this fluid pathway.

The patient’s age and overall health status are important factors in clinical trial eligibility. Many trials for primitive neuroectodermal tumors focus specifically on pediatric patients, as these tumors are more common in children. However, some trials may include young adults. The patient must be healthy enough to tolerate the study treatment, with adequate nutrition and the ability to care for themselves or receive appropriate care.

⚠️ Important

Clinical trial participation requires extensive documentation and testing, but trials offer access to cutting-edge treatments that may not be available otherwise. If your medical team suggests considering a clinical trial, ask detailed questions about what additional testing is required and what the potential benefits and risks might be. The diagnostic tests required for trial enrollment are designed to ensure patient safety and to help researchers understand who benefits most from new treatments.

Previous treatment history affects clinical trial eligibility. Some trials are designed for patients who have not yet received any treatment (called “treatment-naive” patients), while others specifically enroll patients whose tumors have returned after initial treatment. Detailed documentation of any prior surgeries, radiation therapy, or chemotherapy is required during the screening process for clinical trial enrollment.

Performance status assessment is a standard requirement for clinical trials. Doctors use scales that measure how well patients can carry out daily activities. For pediatric patients, doctors assess developmental milestones and functional abilities appropriate for the child’s age. This information helps ensure that patients enrolled in trials have a reasonable chance of tolerating and potentially benefiting from the experimental treatment.

Prognosis and Survival Rate

Prognosis

The prognosis for primitive neuroectodermal tumors depends on several important factors. The location of the tumor plays a significant role, as tumors in certain areas of the brain may be more difficult to remove completely during surgery. The extent of tumor spread at diagnosis is crucial about one-third of patients have tumors that have already spread to other areas at the time they are first diagnosed, which generally indicates a more challenging treatment course.^[1]

The amount of tumor that can be safely removed during surgery significantly affects prognosis. When surgeons can remove all or most of the visible tumor without causing neurological damage, outcomes tend to be better. However, these tumors often grow in areas of the brain that control critical functions, and they can spread in an unpredictable manner, making complete removal difficult.^[9] The age of the patient at diagnosis also influences outcomes, with treatment approaches and prognosis varying between young children, older children, and adults.

The specific molecular characteristics of the tumor, determined through genetic testing, are increasingly recognized as important factors in prognosis. Since 2016, doctors have been classifying these tumors based on their molecular features rather than grouping them all together, and some molecular subtypes appear to have different outcomes than others.^[4] The overall health of the patient and their ability to tolerate aggressive treatment also affects the likely outcome of the disease.

Survival Rate

Determining precise survival rates for primitive neuroectodermal tumors is challenging because the classification of these tumors changed significantly in 2016. Data collected before that time grouped together tumors that are now recognized as distinct diseases with different outcomes. Between 2000 and 2014, approximately 950 people were living with tumors classified as PNETs in the United States. However, the five-year survival rate for adults during that period could not be calculated due to the small number of cases.^[1]

The overall five-year survival rate for the group of tumors formerly called PNETs is reported to be approximately 53 percent, meaning that about half of patients survive at least five years after diagnosis.^[8] However, this figure represents data from before the reclassification of these tumors, and individual survival rates likely vary significantly depending on the specific molecular subtype of the tumor and other patient factors. These tumors are considered serious and require aggressive treatment, but recent medical advances have made cure possible for some patients, particularly children.^[20]

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