Hematology focuses on diseases of the blood, bone marrow, and lymphatic system. Learn about the diagnosis and treatment of anemia, leukemia, and lymphoma.

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Myelodysplastic Syndrome: Diagnosis and Evaluation

Myelodysplastic Syndrome: Diagnosis and Evaluation

Diagnosing Myelodysplastic Syndrome is a meticulous process of exclusion and confirmation. Because the primary symptom—low blood counts—can be caused by simple vitamin deficiencies, infections, or medication side effects, doctors must rule out these reversible causes first. At Liv Hospital, the diagnostic pathway moves from peripheral blood analysis to the gold standard bone marrow examination, followed by advanced molecular profiling to determine the precise subtype and prognosis of the disease.

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Peripheral Blood Analysis

  • The Initial Clues

    The first step is a detailed examination of the blood circulating in the veins.

    Complete Blood Count (CBC)

    This automated test measures the number of red cells, white cells, and platelets. In MDS, at least one of these lines will be low. The test also measures the Mean Corpuscular Volume (MCV), which indicates the size of the red blood cells. In MDS, red blood cells are often macrocytic, meaning they are larger than normal.

    Reticulocyte Count

    This measures young red blood cells. In a healthy person with anemia, the reticulocyte count should be high as the marrow tries to compensate. In MDS, the reticulocyte count is typically inappropriately low, indicating marrow failure.

    Peripheral Blood Smear

    A drop of blood is smeared on a slide and examined under a microscope. Pathologists look for dysplastic changes in the circulating cells, such as neutrophils with hyposegmented nuclei (Pseudo Pelger Huet anomaly) or giant platelets. They also check for the presence of blasts in the blood.

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Ruling Out Reversible Causes

  • The Process of Exclusion

    Before diagnosing a malignancy like MDS, other conditions must be excluded.

    Nutritional Deficiencies

    Low levels of Vitamin B12, folate, or copper can cause blood cells to look dysplastic and mimic MDS. Iron deficiency or chronic kidney disease can also cause anemia.

    Infections and Inflammation

    Chronic viral infections (like HIV or Hepatitis C) or autoimmune disorders can suppress the bone marrow.

    Medications

    Recent use of antibiotics, chemotherapy, or immunosuppressants can cause temporary cytopenias. Doctors carefully review the patient’s drug history.

Bone Marrow Examination

Bone Marrow Examination

The Diagnostic Gold Standard

To confirm MDS, doctors must look directly at the factory where cells are made.

Bone Marrow Aspiration

A needle is inserted into the posterior iliac crest (the back of the hip bone) to suction out the liquid portion of the marrow. This fluid is smeared on slides to assess the morphology (shape) of the developing cells.

Bone Marrow Biopsy

A small core of solid bone and marrow tissue is removed. This allows the pathologist to assess the cellularity—how crowded the marrow is. In MDS, the marrow is usually hypercellular (too many cells) despite the low blood counts, reflecting the ineffective production.

Iron Staining

The marrow sample is stained with Prussian blue dye to look for iron storage. In a specific subtype of MDS, iron accumulates in a ring around the nucleus of the red blood cell precursors. These are called “ring sideroblasts” and are a key diagnostic feature.

Cytogenetic Analysis

Looking at Chromosomes

Looking at Chromosomes

A portion of the marrow aspirate is sent for karyotyping.

Karyotype

This test photographs the chromosomes of the dividing cells. It identifies large structural changes, such as missing chromosomes (monosomy 7) or deleted parts (del 5q). These findings are critical for diagnosis and are the most powerful predictors of the disease course.

FISH (Fluorescence In Situ Hybridization)

If dividing cells are hard to find, FISH can be used to tag specific DNA sequences with fluorescent probes to detect common abnormalities even in resting cells.

Molecular Profiling

Next Generation Sequencing (NGS)

Modern diagnosis increasingly relies on identifying specific gene mutations.

Targeted Panels

Labs use NGS to screen for a panel of genes frequently mutated in MDS, such as SF3B1, TET2, SRSF2, ASXL1, and TP53.

Diagnostic Utility

Finding a mutation can help confirm MDS in difficult cases where the microscopic changes are subtle. For example, finding an SF3B1 mutation strongly supports a diagnosis of MDS with ring sideroblasts.

Prognostic Utility

Some mutations, like TP53, are associated with a more aggressive disease and resistance to standard treatments, while others, like SF3B1, are associated with a better outcome.

Prognostic Scoring Systems

Prognostic Scoring Systems

Predicting the Future

Once the diagnosis is confirmed, patients are stratified by risk to guide treatment.

IPSS R (Revised International Prognostic Scoring System)

This is the standard tool used worldwide. It calculates a score based on five factors:

  1. Percentage of blasts in the bone marrow.
  2. Depth of cytopenias (how low the hemoglobin, platelets, and neutrophils are).
  3. Specific cytogenetic abnormalities (Good, Intermediate, or Poor risk chromosomes).

Risk Groups

Based on the score, patients are classified into five risk groups: Very Low, Low, Intermediate, High, and Very High.

  • Lower Risk: The goal is usually to manage symptoms and improve quality of life.
  • Higher Risk: The goal is to delay progression to leukemia and extend survival, often requiring aggressive treatment.

Differential Diagnosis

Distinguishing Similar Conditions

MDS can look very similar to other bone marrow disorders.

Aplastic Anemia

In aplastic anemia, the marrow is empty (hypocellular) and the cells are not dysplastic; they are just absent. In MDS, the marrow is usually full.

Acute Myeloid Leukemia (AML)

The distinction is based on the blast count. If blasts are <20%, it is MDS. If >20%, it is AML.

Myeloproliferative Neoplasms (MPN)

In these disorders, the marrow produces too many effective cells (high counts), whereas in MDS, it produces too many ineffective cells (low counts). There is also an overlap category called MDS/MPN (e.g., CMML) where patients have features of both.

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FREQUENTLY ASKED QUESTIONS

Is a bone marrow biopsy painful?

It is performed under local anesthesia to numb the skin and bone surface. Most patients feel pressure and a brief sharp sensation during aspiration, but it is generally well tolerated and quick.

Genetic testing tells doctors how aggressive the MDS is. This helps decide if you need a stem cell transplant or if you can be managed with milder treatments.

It is an immature red blood cell with a ring of iron deposits around its nucleus. Seeing these in the marrow helps doctors diagnose a specific, usually milder, type of MDS.

It means the bone marrow is packed full of cells. In MDS, this is a sign that the marrow is trying hard to make blood, but the cells are dying before they get out.

No. While blood tests can strongly suggest MDS, a bone marrow biopsy is required to see the dysplastic cells and check genetics for a final confirmation.

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