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Inflammatory myofibroblastic tumour – Diagnostics

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Diagnosing inflammatory myofibroblastic tumour involves a combination of imaging techniques, tissue analysis, and molecular testing to distinguish this rare condition from other tumours and infections, helping doctors determine the most appropriate treatment approach.

Introduction: When to Seek Diagnostic Evaluation

Inflammatory myofibroblastic tumour (IMT) presents a unique challenge because it can develop without causing noticeable symptoms for quite some time. Many people discover they have this condition during routine health checkups or when investigating unrelated concerns.[1] The tumour can grow silently until it reaches a size that begins to interfere with nearby organs or structures, at which point symptoms become apparent.[1]

If you experience persistent symptoms such as unexplained fever, night sweats, unintentional weight loss, or a general feeling of unwellness that doesn’t go away, it’s important to seek medical attention.[12] These symptoms can mimic many other conditions, including infections or other types of tumours, which is why proper diagnostic testing is essential. Pain at a specific location in the body, particularly if it’s associated with a lump or mass that can be felt, should also prompt a visit to your doctor.[12]

The symptoms you experience will largely depend on where the tumour is located and how large it has grown.[8] For instance, if an IMT develops in the lungs, you might have a cough, difficulty breathing, or chest pain that feels similar to a respiratory infection.[15] If the tumour is in the abdomen, you might feel abdominal pain or notice a mass during physical examination.[13] Because IMT occurs most commonly in children and young adults, any unusual symptoms in this age group warrant careful evaluation.[1]

⚠️ Important
Some patients with inflammatory myofibroblastic tumour remain completely symptom-free until the tumour is discovered incidentally during imaging tests for other reasons. Don’t ignore persistent, unexplained symptoms even if they seem mild, especially if you’re a child, teenager, or young adult, as early detection can improve treatment outcomes.

Diagnostic Methods for Identifying IMT

Imaging Studies

When doctors suspect an inflammatory myofibroblastic tumour, they typically begin with imaging studies to locate the mass and understand its characteristics. Computed tomography, commonly called a CT scan, is one of the primary imaging tools used to evaluate IMT.[1] This test creates detailed cross-sectional images of the body that help doctors determine the tumour’s size, exact location, and whether it has spread to surrounding tissues.[13]

For tumours in the lungs, a chest CT scan will show a mass that is typically large, peripherally located, and lobulated in appearance.[10] The tumour may show signs of invading the chest wall, blood vessels, or structures in the middle of the chest called the mediastinum. Sometimes calcification—deposits of calcium that appear bright white on the scan—can be seen within the tumour.[10] When contrast dye is injected during the scan, IMTs typically show a heterogeneous pattern of enhancement, meaning some areas light up more than others.[10]

Magnetic resonance imaging, or MRI, is another imaging technique that can be useful, particularly for tumours in certain locations.[10] MRI uses powerful magnets and radio waves instead of radiation to create detailed images of soft tissues. When an MRI is performed on an IMT, the tumour may appear similar in brightness to skeletal muscle, though the appearance can vary.[10]

Ultrasound imaging may be employed for tumours in the abdomen or pelvis, as it can help visualize soft tissue masses and their relationship to nearby organs without using radiation.[2] For abdominal IMTs, ultrasound or CT scans can reveal a soft tissue mass that may be pressing on or surrounding important blood vessels or organs.[13]

Advanced Imaging: PET Scans

In some cases, doctors may order a specialized test called positron emission tomography, or PET scan, often combined with a CT scan (PET-CT).[17] This test uses a small amount of radioactive glucose that is injected into your bloodstream. Cancer cells and some inflammatory cells take up this glucose more readily than normal cells, causing them to light up on the scan. This test helps doctors understand how active the tumour is.

However, PET scans can be confusing when evaluating IMT because these tumours contain many inflammatory cells. The amount of radioactive glucose uptake by an IMT can vary considerably depending on factors like how densely packed the cells are, how quickly they’re dividing, and how many plasma cells (a type of white blood cell) are present.[15] This means that an IMT can sometimes look very “hot” or active on a PET scan, making it difficult to distinguish from a malignant tumour based on imaging alone.[17]

Biopsy: The Gold Standard for Diagnosis

While imaging studies can show that a mass is present and provide information about its characteristics, they cannot definitively determine whether the tumour is an IMT or something else. To make an accurate diagnosis, doctors need to examine the actual tumour cells under a microscope, which requires taking a sample through a procedure called a biopsy.[12]

There are different ways to obtain a biopsy sample. For tumours that are easily accessible, a doctor may perform a needle biopsy, using a thin needle to remove a small sample of tissue.[17] This procedure is often guided by CT scanning or ultrasound to ensure the needle reaches the correct location.[17] However, because IMTs can have variable appearances and the needle samples are small, they may not always provide enough tissue to make a confident diagnosis.[15]

For lung tumours, doctors might attempt to obtain samples through bronchoscopy, a procedure where a flexible tube with a camera is inserted through the mouth or nose and into the airways.[17] However, this approach may not always reach the tumour if it’s located on the outer edges of the lung, and even when samples are obtained, the small amount of tissue may not be representative of the entire tumour.[15]

In many cases, the most reliable way to diagnose IMT is through surgical biopsy or complete surgical removal of the tumour.[1] This provides pathologists with enough tissue to thoroughly examine the tumour’s characteristics and perform additional specialized tests. The surgical approach allows doctors to see the tumour in its entirety and understand how it relates to surrounding structures.[15]

Microscopic Examination and Pathology

Once tissue is obtained, a specialist called a pathologist examines it under a microscope. IMTs have a distinctive appearance characterized by spindle-shaped cells that are longer than they are wide, mixed with numerous inflammatory cells.[1] The inflammatory cells are predominantly plasma cells and lymphocytes, which are types of white blood cells, along with some eosinophils—cells typically involved in allergic reactions and parasite infections.[1]

The spindle cells in IMT are special cells called myofibroblasts, which have features of both fibroblasts (cells that produce connective tissue) and smooth muscle cells.[2] These cells help maintain the structure of organs and play a role in wound healing, but in IMT they grow abnormally. The pathologist will look for these characteristic cells scattered throughout tissue that contains abundant inflammatory cells.[1]

To confirm the diagnosis, pathologists use special staining techniques that highlight specific proteins in the tumour cells. They may test for markers such as CD68 and vimentin, which are typically present in myofibroblastic cells.[15] These additional tests help distinguish IMT from other conditions that might look similar under the microscope, such as infections, reactive inflammatory conditions, or other types of tumours.[1]

Molecular and Genetic Testing

One of the most important advances in diagnosing IMT has been the discovery that many of these tumours have specific genetic abnormalities. In approximately 50 to 80 percent of IMT cases, there is a rearrangement involving a gene called ALK, which stands for anaplastic lymphoma kinase.[5][8] This means that pieces of chromosomes—the structures in cells that contain genes—break apart and reconnect in abnormal ways.

When the ALK gene is rearranged, it fuses with other genes to create what scientists call fusion proteins. These abnormal proteins can drive the tumour’s growth.[2] Pathologists can detect ALK protein in tumour tissue using a special staining technique called immunohistochemistry, which makes the ALK protein visible under the microscope.[8] Finding ALK positivity not only helps confirm the diagnosis but also provides crucial information about treatment options, as there are now medications specifically designed to block these abnormal ALK proteins.[3]

Some IMTs don’t have ALK rearrangements but instead have abnormalities in other genes such as ROS1, NTRK3, RET, or PDGFRB.[10] Comprehensive molecular testing can identify these alternative genetic changes, which is particularly important because different genetic abnormalities may respond to different targeted treatments.[3] In more than 90 percent of children with IMT, genetic abnormalities such as ALK gene rearrangement or ROS1 gene fusions can be identified.[3]

Laboratory Blood Tests

While there is no single blood test that can diagnose IMT, certain laboratory findings may provide supporting evidence. Some patients with IMT have abnormal blood counts, including elevated levels of white blood cells or platelets.[17] Others may show increased levels of certain proteins in the blood, such as polyclonal gamma-globulin, or elevated inflammatory markers like interleukin-6 (IL-6) and interleukin-1 beta (IL-1β).[17]

However, these findings are not specific to IMT and can occur with many other conditions, including infections and different types of tumours.[17] Therefore, blood tests are used as part of the overall clinical picture rather than as definitive diagnostic tools. They may be more helpful in monitoring the tumour’s response to treatment or detecting recurrence after treatment.

Diagnostics for Clinical Trial Qualification

When patients with IMT are being considered for enrollment in clinical trials, they typically need to undergo a more extensive evaluation beyond the standard diagnostic workup. Clinical trials have specific criteria that participants must meet to ensure the study can safely and accurately assess new treatments.

One of the most critical requirements for many clinical trials involving IMT is confirmation of the tumour’s molecular profile, particularly ALK status.[10] Trials testing ALK-targeted medications require documented evidence that the tumour is ALK-positive through either immunohistochemistry or more sophisticated genetic testing methods such as fluorescence in situ hybridization (FISH) or next-generation sequencing.[10] These molecular diagnostic techniques identify the specific genetic rearrangement present in the tumour cells.

Patients being screened for clinical trials usually need comprehensive imaging to establish a baseline measurement of the tumour and to confirm that it hasn’t spread to distant organs.[8] This baseline is crucial because it allows researchers to accurately measure whether the treatment is shrinking the tumour or slowing its growth. Imaging studies may include CT scans of the chest, abdomen, and pelvis, as well as MRI scans of specific areas depending on where the tumour is located.

Clinical trials may also require tissue samples to be sent to specialized laboratories for additional molecular analysis. This can include testing for gene fusions beyond ALK, looking at the tumour’s complete genetic profile, or analyzing specific biomarkers that might predict how well the tumour will respond to the experimental treatment.[11] Some trials collect fresh biopsy samples rather than using previously obtained tissue to ensure the molecular testing is as accurate and up-to-date as possible.

Blood tests are another standard component of clinical trial screening. These establish that patients have adequate organ function—particularly liver, kidney, and bone marrow function—to safely receive the experimental treatment.[11] Researchers need to ensure that participants can metabolize and clear the study medication from their bodies and that they have sufficient blood cell counts to tolerate potential side effects.

Eligibility criteria often specify whether the IMT must be unresectable, meaning it cannot be safely removed by surgery, or whether it has recurred after previous treatment.[10] This determination requires careful review of imaging studies by experienced surgeons and radiologists to confirm that surgical removal is not feasible or would not be in the patient’s best interest. Some trials specifically enroll patients whose tumours have progressed despite previous therapies, requiring documentation of treatment history and disease progression.

Age restrictions are common in clinical trials for rare tumours like IMT. Some studies focus exclusively on pediatric patients, while others include both children and adults.[11] Documentation of the patient’s age and, for children, measurements of growth and developmental stage may be required. Patients or their legal guardians must also be able to understand and consent to participate in the trial, which involves additional documentation and educational processes.

⚠️ Important
Enrollment in clinical trials requires extensive molecular testing that may not be part of standard diagnostic procedures. If you’re interested in participating in a clinical trial, ask your doctor about having your tumour tissue tested for ALK and other gene rearrangements early in the diagnostic process, as this information may open up additional treatment options.

Prognosis and Survival Rate

Prognosis

The prognosis for patients with inflammatory myofibroblastic tumour is generally favorable, but several factors influence the expected outcome.[1] The anatomical location of the tumour plays a significant role—tumours that can be completely removed surgically tend to have excellent outcomes, while those in locations that make complete removal difficult or impossible may present more challenges.[1]

Complete surgical resection is one of the most important factors determining prognosis. Patients whose tumours are entirely removed have the best chance of cure.[10] However, IMT has a tendency to recur locally, with recurrence rates of approximately 25 percent reported in various studies.[8] The risk of recurrence is particularly high when the tumour is located in the abdominal cavity or when it is larger than 8 centimeters.[8]

One encouraging aspect of IMT is that distant metastasis—spread to organs far from the original tumour—is rare. Most studies report that metastasis occurs in only about 5 to 10 percent of cases.[2][8] Interestingly, metastasis appears to be more common in tumours that are ALK-negative, meaning they don’t have the ALK gene rearrangement.[8] Younger age, larger tumour size, and tumours located in the abdomen, pelvis, or lungs have been associated with higher metastatic potential.[8]

Tumor size and patient age also influence outcomes. Younger patients, particularly children, and those with tumours smaller than 6.5 centimeters tend to have better survival rates.[8] The development of targeted therapies, particularly medications that block abnormal ALK proteins, has improved the outlook for patients with unresectable or recurrent disease.[3][8]

Survival Rate

While exact survival statistics for inflammatory myofibroblastic tumour can be difficult to establish due to its rarity, available data suggest that most patients have good long-term outcomes, especially when the tumour can be completely removed surgically.[1] One study reported five-year overall survival rates of 85.7 percent and event-free survival rates of 72.9 percent for children with IMT.[11]

Patients who achieve complete surgical resection with negative margins—meaning no tumour cells are seen at the edges of the removed tissue—have excellent prognosis.[10] Even when the tumour cannot be completely removed or when it recurs, newer targeted therapies have shown promising results. Some patients with unresectable tumours treated with medications like crizotinib have achieved complete remission, meaning no evidence of tumour remains on imaging studies.[11]

It’s important to note that IMT behaves differently than most cancers. While it is classified as a tumour with intermediate malignant potential, meaning it has some features of both benign and malignant tumours, its behavior is generally less aggressive than most cancers.[2] The main concerns are local recurrence and the rare possibility of distant spread, rather than the rapid progression seen with many malignancies. Long-term follow-up is important because recurrences can occur even years after initial treatment.[1]

Ongoing Clinical Trials on Inflammatory myofibroblastic tumour

  • Study of Brigatinib for Children and Young Adults with ALK+ Anaplastic Large Cell Lymphoma, Inflammatory Myofibroblastic Tumors, or Other Solid Tumors

    Recruiting

    1 1 1 1
    Investigated diseases:
    Investigated drugs:
    Austria Belgium Czechia Denmark Finland France +6

  • Study of Crizotinib and Temsirolimus for Children with ALK, ROS1, or MET Positive Cancers, Including Neuroblastoma and Rhabdomyosarcoma

    Recruiting

    1 1 1 1
    Investigated diseases:
    Investigated drugs:
    Denmark Finland France Germany Italy The Netherlands +3

References

https://pmc.ncbi.nlm.nih.gov/articles/PMC12026078/

https://en.wikipedia.org/wiki/Inflammatory_myofibroblastic_tumour

https://www.texaschildrens.org/content/conditions/inflammatory-myofibroblastic-tumor

https://www.cancer.gov/publications/dictionaries/cancer-terms/def/inflammatory-myofibroblastic-tumor

https://pmc.ncbi.nlm.nih.gov/articles/PMC9367282/

https://pubmed.ncbi.nlm.nih.gov/37394916/

https://pmc.ncbi.nlm.nih.gov/articles/PMC3531700/

https://link.springer.com/article/10.1007/s11864-023-01144-6

https://bmcpulmmed.biomedcentral.com/articles/10.1186/s12890-024-02873-6

https://www.cancer.gov/types/lung/hp/child-pulmonary-inflammatory-myofibroblastic-tumor-treatment-pdq

https://turkjpediatr.org/article/view/5463

https://www.cancer.gov/pediatric-adult-rare-tumor/rare-tumors/rare-soft-tissue-tumors/inflammatory-myofibroblastic-tumor

https://pmc.ncbi.nlm.nih.gov/articles/PMC3531700/

https://www.youtube.com/watch?v=tgMJIZqa2Ro

https://jovs.amegroups.org/article/view/22011/html

https://pmc.ncbi.nlm.nih.gov/articles/PMC12026078/

https://bmcpulmmed.biomedcentral.com/articles/10.1186/s12890-024-02873-6

https://www.facebook.com/groups/1506464572901654/posts/3767498583464897/

https://medlineplus.gov/diagnostictests.html

https://www.questdiagnostics.com/

https://www.healthdirect.gov.au/diagnostic-tests

https://www.who.int/health-topics/diagnostics

https://www.yalemedicine.org/clinical-keywords/diagnostic-testsprocedures

https://www.nibib.nih.gov/science-education/science-topics/rapid-diagnostics

https://www.health.harvard.edu/diagnostic-tests-and-medical-procedures

https://www.roche.com/stories/terminology-in-diagnostics

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Inflammatory myofibroblastic tumour:

FAQ

Can inflammatory myofibroblastic tumour be diagnosed with a simple blood test?

No, there is no specific blood test that can diagnose inflammatory myofibroblastic tumour. While some patients may have abnormal blood findings such as elevated white blood cells, platelets, or inflammatory markers like IL-6, these changes are not specific to IMT and can occur with many other conditions. A definitive diagnosis requires tissue examination through biopsy, where a pathologist can identify the characteristic spindle cells and inflammatory infiltrate under a microscope, often combined with molecular testing for gene rearrangements like ALK.[17][12]

What does it mean if my IMT is ALK-positive?

ALK-positive means that your tumour has a rearrangement in the ALK (anaplastic lymphoma kinase) gene, which occurs in approximately 50 to 80 percent of IMT cases. This genetic change causes the tumour cells to produce abnormal fusion proteins that drive tumour growth. The good news is that ALK-positive status opens up treatment options with targeted medications called ALK inhibitors, such as crizotinib, which specifically block these abnormal proteins. These targeted therapies have shown promising results in treating unresectable or recurrent IMTs and have fewer side effects than traditional chemotherapy.[5][8][3]

Why do doctors need a biopsy if imaging already shows a tumour?

Imaging studies like CT scans, MRI, or PET scans can show that a mass is present and provide information about its size and location, but they cannot definitively determine what type of tumour it is. Inflammatory myofibroblastic tumours can look similar to infections, other benign tumours, or even cancers on imaging studies. A biopsy provides actual tumour tissue that pathologists can examine under a microscope to identify the characteristic cells and inflammatory patterns of IMT. Additionally, the biopsy tissue allows for molecular testing to determine if ALK or other gene rearrangements are present, which is crucial for planning treatment.[12][15]

How accurate is needle biopsy for diagnosing inflammatory myofibroblastic tumour?

Needle biopsies can be helpful but may not always provide a definitive diagnosis of IMT. Because these tumours can have variable appearances in different areas and because needle biopsies collect only small tissue samples, the sample may not be representative of the entire tumour. The small amount of tissue obtained might not contain enough of the characteristic spindle cells and inflammatory infiltrate needed for diagnosis. In many cases, surgical biopsy or complete removal of the tumour is the most reliable way to diagnose IMT, as it provides pathologists with enough tissue to thoroughly examine all features and perform comprehensive molecular testing.[15]

Do all patients with IMT need molecular testing for gene rearrangements?

Yes, molecular testing for gene rearrangements, particularly ALK, is highly recommended for all patients diagnosed with inflammatory myofibroblastic tumour. This testing is important for several reasons: it helps confirm the diagnosis, provides prognostic information (ALK-positive tumours appear to metastasize less frequently), and most importantly, identifies patients who may benefit from targeted therapies. If your tumour is ALK-positive and cannot be completely removed surgically or if it recurs after surgery, you may be eligible for treatment with ALK inhibitors. Additionally, some clinical trials require documented molecular testing results for enrollment, so having this information early in your diagnosis can open up additional treatment options.[3][10][11]

🎯 Key takeaways

  • Inflammatory myofibroblastic tumour is often discovered incidentally during routine health checks or when investigating symptoms like fever, weight loss, and localized pain that can mimic infections or other conditions.
  • Imaging studies like CT scans and MRI can show the tumour’s location and size but cannot definitively distinguish IMT from other tumours or infections—tissue examination is essential for diagnosis.
  • Biopsy is the gold standard for diagnosing IMT, revealing characteristic spindle-shaped myofibroblastic cells mixed with abundant inflammatory cells including plasma cells and lymphocytes.
  • Molecular testing for ALK gene rearrangements and other genetic abnormalities is crucial because it confirms diagnosis, predicts behavior, and identifies patients who can benefit from targeted therapies.
  • About 50 to 80 percent of IMTs are ALK-positive, meaning they have genetic changes that can be targeted with specific medications like crizotinib, offering new hope for unresectable tumours.
  • More than 90 percent of children with IMT have identifiable genetic abnormalities in their tumour tissue, making molecular diagnostics particularly important in pediatric cases.
  • Clinical trial enrollment requires extensive molecular profiling beyond standard diagnostics, so requesting comprehensive genetic testing early in diagnosis may open additional treatment opportunities.
  • Prognosis is generally favorable when tumours are completely removed surgically, with most patients having good long-term outcomes despite a 25 percent local recurrence rate.

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