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Myeloid Neoplasms

Neoplasms originating from hematopoietic progenitors, known as myeloid neoplasms, typically result in clonal proliferations that replace the normal cells in the bone marrow.

AML: Pathology | Medical Science Optional Notes for UPSC

AML-FAB Classification

AML: Pathology | Medical Science Optional Notes for UPSC

AUER Rods

  • Auer rods are unique rod-like structures that stain red and may be found in myeloblasts or cells at more advanced stages of differentiation.
  • They are notably abundant in cases of acute promyelocytic leukemia.

Auer rods are indicative of neoplastic myeloblasts, serving as a valuable diagnostic indicator when detected.

Question for AML: Pathology
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Which unique structures are indicative of neoplastic myeloblasts and are notably abundant in cases of acute promyelocytic leukemia?
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AML-WHO Classification

Acute myeloid leukemias (AMLs) exhibit diversity in terms of genetics, cellular lineage, and maturation levels. The World Health Organization (WHO) classification utilizes these features to categorize AML into four groups:

  1. AMLs linked to specific genetic abnormalities, crucial for predicting outcomes and guiding therapy.
  2. AMLs displaying dysplasia, many of which originate from myelodysplastic syndromes.
  3. AMLs emerging post-genotoxic chemotherapy.
  4. AMLs without the aforementioned features.

AMLs falling into the last category are further classified based on the predominant line of differentiation observed in the tumor.

AML: Pathology | Medical Science Optional Notes for UPSC

AML-Etiology

Environmental Influences

  • Benzene
  • Ionizing radiation
  • Tobacco, chemotherapy drugs

Genetic or Chromosomal Contributors

  • Down syndrome
  • t(15;17) translocation (notably associated with acute promyelocytic leukemia (M3))
  • Fanconi anemia
  • Philadelphia translocation (observed in less than 2% of AML patients)

AML-M31 (15;17)

The translocation t(15;17) leads to the fusion of the retinoic acid receptor alpha (RARA) gene on chromosome 17 with the PML gene on chromosome 15. This fusion results in the formation of a PML/RARalpha chimeric gene, generating a fusion protein that hinders myeloid differentiation at the promyelocytic stage, potentially by inhibiting the normal function of retinoic acid receptors.

Interestingly, therapeutic doses of all-trans retinoic acid (ATRA), an analog of vitamin A, can overcome this differentiation block, prompting the neoplastic promyelocytes to swiftly differentiate into neutrophils. As neutrophils have an average lifespan of about 6 hours, ATRA treatment rapidly eliminates the tumor.

Recent observations indicate that combining ATRA with arsenic trioxide, a substance that induces the degradation of the PML/RARA fusion protein, is more effective than ATRA alone. This combination achieves cures in over 80% of patients.

AML-Prognostic Factors

AML: Pathology | Medical Science Optional Notes for UPSC

Question for AML: Pathology
Try yourself:
What is the main characteristic of AMLs falling into the category without specific genetic abnormalities or dysplasia?
View Solution

AML - Repeats

Give the FAB classification of acute myeloid leukemia and discuss the laboratory findings in a case of M3 AML. (2012)

The document AML: Pathology | Medical Science Optional Notes for UPSC is a part of the UPSC Course Medical Science Optional Notes for UPSC.
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FAQs on AML: Pathology - Medical Science Optional Notes for UPSC

1. What is the AML-FAB classification?
Ans. The AML-FAB classification is a system used to classify acute myeloid leukemia (AML) based on the morphology and cytochemistry of the leukemia cells. It was developed by the French-American-British (FAB) Cooperative Group and classifies AML into eight subtypes (M0 to M7) based on distinct features observed under the microscope.
2. What are AUER rods in the context of myeloid neoplasms?
Ans. AUER rods are needle-like structures that are observed in the cytoplasm of myeloid cells during the examination of bone marrow or blood smears. They are a characteristic feature of acute myeloid leukemia (AML) and are often used as a diagnostic marker. AUER rods consist of abnormal granules formed by the fusion of primary granules within the leukemia cells.
3. What is the AML-WHO classification?
Ans. The AML-WHO classification is a system used to classify acute myeloid leukemia (AML) based on the genetic and molecular abnormalities of the leukemia cells. It was developed by the World Health Organization (WHO) and provides a more comprehensive understanding of the disease compared to the AML-FAB classification. The AML-WHO classification includes several subcategories based on specific genetic mutations and chromosomal abnormalities.
4. What is the etiology of AML?
Ans. The etiology of acute myeloid leukemia (AML) is multifactorial and can involve both genetic and environmental factors. Some common risk factors for AML include exposure to high levels of radiation, certain genetic disorders (such as Down syndrome), previous chemotherapy or radiation therapy for other cancers, exposure to certain chemicals (such as benzene), and certain genetic mutations (such as FLT3-ITD and NPM1 mutations). However, in many cases, the exact cause of AML is unknown.
5. What are the pathological features of AML?
Ans. The pathological features of acute myeloid leukemia (AML) include the excessive proliferation of abnormal myeloid cells in the bone marrow, leading to a decrease in the production of normal blood cells. The leukemia cells in AML often have abnormal morphology, such as increased cytoplasmic granules and irregular nuclear shape. These cells can infiltrate other organs and tissues, leading to organ dysfunction. The specific genetic and molecular abnormalities present in the leukemia cells can also vary, contributing to the heterogeneity of AML.
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