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Pre-leukemia
Dr. Akshay Agarwal
Moderator : Dr. Sangeeta Sharma
Introduction
Pre-leukemia are a group of disorders that most
commonly present with cytopenia(s) and has a
tendency to progress into acute leukemias unless
attended to clinically.
These include Myeloproliferative syndromes,
Marrow failure syndromes and congenital defects.
Disorders implicated in the
Pathogenesis of AML
Marrow Failure Syndromes Congenital Defects
Myelodysplastic Syndrome Down’s Syndrome
Fanconi’s Anemia Bloom Syndrome
Shwachman-Diamond Syndrome Monosomy 7 syndrome
Amegakaryocytic Thrombocytopenia Klinefelter Syndrome
Blackfan-Diamond Syndrome Turner Syndrome
Kostmann Agranulocytosis Neurofibromatosis
Familial Aplastic Anemia Congenital Dysmorphic syndromes
Dyskeratosis Congenita
Myelodysplastic Syndrome
• Derived from 2 words:
• Myelo – the Myeloid series
• Dysplastic – dysplasia meaning disordered
growth
Dysplastic features of
Erythroid series
• Megaloblastosis
• Karyorrhexis
• Nuclear irregularity
• Fragmentation or multinucleation
• Ring Sideroblasts
• Cytoplasmic Vacuoles
• PAS positivity
Iron stain
Dysplastic features of
Granulocytic series
• Hypogranular neutrophil
• Pseudo-Pelger Huet anomaly
• Bizzare segmented neutrophils
Dysplastic features of
Megakaryocytic series
• Micromegakaryocytes
• Non lobated or multiple nuclei
• The myelodysplastic syndromes (MDSs) are
disorders caused by a clonal expansion of
hematopoietic stem cells in which maturation is
abnormal (dysplastic) and production ineffective,
resulting in many cells being destroyed before they
reach the systemic circulation. Anemia typically
occurs, often accompanied by thrombocytopenia
and/or neutropenia. Some cases develop from
exposure to ionizing radiation or cytotoxic
chemotherapy, usually with alkylating agents, and in
these circumstances the bone marrow is
characteristically hypocellular and partially fibrotic
Classification
Sr.
No.
Disease Blood findings Bone marrow findings
1 Refractory cytopenias with unilineage dysplasia
(RCUD)
Uni / bi-cytopenias
No or rare blasts (<1%)
Unilineage dysplasia: >
10% of the cells in one
myeloid lineage
<5% blasts
<15% of erythroid
precursors are ring
sideroblasts
2 Refractory anemia with ring siderblasts (RARS) Anemia
No blasts
>15% of erythroid
precursors are ring
sinderblasts
Erythroid dysplasia only
<5% blasts
3 Refractory cytopenia with multilineage
dysplasia
(RCDM)
Cytopenia(s)
No or rare blasts
No Auer rods
<1 x 109/L monocytes
Dysplasia in >10% of the
cells in >2 myeloid
lineages
<5% blasts
No auer rods
+/- 15% ring sideroblasts
Sr.
No.
Disease Blood findings Bone marrow findings
4 Refractory Anemia with excess blasts -1
(RAEB-1)
Cytopenia
<5% blasts
No auer rods
<1 x 109/L monocytes
Unilineage or
multilineage dysplasia
5-9% blasts
No auer rods
5 Refractory Anemia with excess blasts -2
(RAEB -2)
Cytopenia
5-19% blasts
+/- auer rods
<1 x 109/L monocytes
Unilineage or
multilineage dysplasia
10-19% blasts
+/- auer rods
6. Myelodysplastic syndrome – unclassified
(MDS-U)
Cytopenia
<1% blasts
Unequivocal dysplasis
in ,10% cells
<5% blasts
7. MDS associated with isolated del (5q) Anemia
Normal to increased
platelet count
No or rare blasts
Normal to increased
megakaryocytes with
hypolobated nuclei
<5% blasts
Isolated del(5q)
No auer rods
Fanconi’s Anemia
• Autosomal recessive
• FA is the result of a genetic defect in a cluster of
proteins responsible for a DNA repair.
• As a result, the majority of FA patients develop
cancer, most often acute myelogenous leukemia
in 33%, and 90% develop bone marrow failure by
the age of 40.
• Most commonly M4 (Myelomonocytic) and M5
(monocytic)
• Significant risk of solid tumors like
• Hepatic tumors
• Squamous cell carcinoma
• 28% calculated risk by the age 40
Cell and Molecular Biology
• FA cells characteristically display a high frequency of
spontaneous chromosomal breakage and
hypersensitivity to DNA cross-linking agents.
• A subset of patients also present with biallelic
mutations in BRCA2 gene
• BRCA2 protein is important in the repair of DNA
damage.
• Thus, cells lacking BRCA2 inaccurately repair
damaged DNA and are hypersensitive to DNA
crosslinking agents.
Signs and Symptoms
• During childhood, short stature and skin pigmentation,
including café au lait spots, may become apparent.
• The first sign of a hematologic problem is usually
petechiae and bruises, with later onset of pale
appearance, feeling tired, and infections.
• Somatic abnormalities such as Skeletal (absent
thumbs, radial hypoplasia, scoliosis), genitourinary (
inferitility, horseshoe kidneys) , gastrointestinal,
cardiac and neurological may be present
Bilateral thumb hypoplasia
Treatment
• Administration of oxymetholone, corticosteroids
can show response in upto 70% patients but
many will become refractory after variable time
• Hematopoietic stem cell transplant is the
treatment of choice.
Dyskeratosis Congenita
• X-linked recessive, autosomal dominant and
autosomal recessive forms
• Bone marrow failure develops below the age of
20 years; 80-90% will develop bone marrow
abnormalities by age 30 yrs.
Cell and Molecular Biology
• Peripheral blood and bone marrow metaphases from
patients show unbalanced chromosomal
rearrangements in the absence of any clastogenic
agents
• Chromosome/genomic instability
• Defect in DKC1 gene leading to defective ribosome
production
• Hematopoietic progenitor studies have shown
reduced numbers of all progenitors.
Signs and Symptoms
• Characterized by the mucocutaneous triad of
abnormal skin pigmentation, nail dystrophy and
mucosal leucoplakia
• Bone marrow failure is the principal cause of
early mortality with an early predisposition to AML
• Non-cutaneous lesions such as short stature,
pulmonary disease, esophageal strictures have
been documented.
Treatment
• Transient successful responses to
granulocyte/macrophage colony-stimulating
factor, Granulocyte colony-stimulating factor and
erythropoietin have been reported
• Steroid oxymetholone
• Hematopoietic Stem cell transplant
Shwachman-Diamond
Syndrome
• Shwachman–Diamond syndrome is characterized
by an autosomal recessive mode of inheritance.
The gene that is mutated in this syndrome lies on
the long arm of chromosome 7 at cytogenetic
position 7q11
• rare congenital disorder characterized by
exocrine pancreatic insufficiency, bone marrow
dysfunction, skeletal abnormalities, and short
stature. After cystic fibrosis (CF), it is the second
most common cause of exocrine pancreatic
insufficiency in children.
Cell and Molecular biology
• The SDS gene is on 7q11.22 which is mutated in
90% patients.
• Its importance in indicated in RNA metabolism
and ribosome biogenesis.
Hematological
abnormalities
• Neutropenia - Low neutrophil counts leave patients at
risk of developing severe recurrent infections that
may be life-threatening.
• Anemia and thrombocytopenia may also occur. Bone
marrow is typically hypocellular, with maturation
arrest in the myeloid lineages that give rise to
neutrophils, macrophages, platelets and red blood
cells.
• Patients may also develop progressive marrow failure
or transform to acute myelogenous leukemia.
Treatment
• G-CSF
• Incidence of myelodysplasia and transformation
to AML is seen in 15-25%
• Particularly AML with erythroid differentiation: M6
Blackfan-Diamond
Syndrome
• Most pedigrees suggest an autosomal dominant
mode of inheritance with incomplete penetrance.
Approximately 10–25% of DBA occurs with a
family history of disease.
• Inherited pure red cell aplasia is a congenital
erythroid aplasia that usually presents in infancy.
• DBA causes anemia, without substantially
affecting the other blood
Diagnostic criteria
• Normochromic macrocytic Anemia
• Reticulocytopenia
• Normocellular bone marrow with selective
deficiency of erythroid precursors
• Decreased leukocyte counts with normal to
increased platelet counts
• Elevated erythrocyte deaminase activity
Kostmann Agranulocytosis
• Kostmann disease is a form of severe congenital
neutropenia which is a rare autosomal recessive
condition in which severe chronic neutropenia is
detected soon after birth.
Diagnosis
• An absolute neutrophil count chronically less than 500/mm3,
usually less than 200/mm3, is the main sign of Kostmann's.
• Other elements include the severity of neutropenia, and other
normal findings (hemoglobin, platelets)
• Isolated neutropenia in infants can occur in viral infections,
autoimmune neutropenia of infancy, bone marrow suppression
from a drug or toxin, hypersplenism, and passive placental
transfer of maternal IgG
• The bone marrow usually shows early granulocyte precursors,
but myelopoietic development stops at the promyelocyte and/or
myelocyte stage, so that few maturing forms are seen.
Bloom Syndrome
• are autosomal recessive disorder characterized
by short stature, caused by mutations in the BLM
gene leading to mutated DNA helicase protein
formation.
Signs and Symptoms
• short stature and a rash on the face
• moderate immune deficiency, characterized by
deficiency in certain immunoglobulin classes and
apparently leading to recurrent pneumonia and ear
infections.
• low birth weight
• Hypogonadism is characterized by a failure to
produce sperm, hence infertility in males, and
premature cessation of menses (premature
menopause)
• Thank you

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Pre leukemia MDS

  • 2. Introduction Pre-leukemia are a group of disorders that most commonly present with cytopenia(s) and has a tendency to progress into acute leukemias unless attended to clinically. These include Myeloproliferative syndromes, Marrow failure syndromes and congenital defects.
  • 3. Disorders implicated in the Pathogenesis of AML Marrow Failure Syndromes Congenital Defects Myelodysplastic Syndrome Down’s Syndrome Fanconi’s Anemia Bloom Syndrome Shwachman-Diamond Syndrome Monosomy 7 syndrome Amegakaryocytic Thrombocytopenia Klinefelter Syndrome Blackfan-Diamond Syndrome Turner Syndrome Kostmann Agranulocytosis Neurofibromatosis Familial Aplastic Anemia Congenital Dysmorphic syndromes Dyskeratosis Congenita
  • 4. Myelodysplastic Syndrome • Derived from 2 words: • Myelo – the Myeloid series • Dysplastic – dysplasia meaning disordered growth
  • 5. Dysplastic features of Erythroid series • Megaloblastosis • Karyorrhexis • Nuclear irregularity • Fragmentation or multinucleation • Ring Sideroblasts • Cytoplasmic Vacuoles • PAS positivity
  • 6.
  • 8. Dysplastic features of Granulocytic series • Hypogranular neutrophil • Pseudo-Pelger Huet anomaly • Bizzare segmented neutrophils
  • 9.
  • 10.
  • 11.
  • 12. Dysplastic features of Megakaryocytic series • Micromegakaryocytes • Non lobated or multiple nuclei
  • 13.
  • 14.
  • 15. • The myelodysplastic syndromes (MDSs) are disorders caused by a clonal expansion of hematopoietic stem cells in which maturation is abnormal (dysplastic) and production ineffective, resulting in many cells being destroyed before they reach the systemic circulation. Anemia typically occurs, often accompanied by thrombocytopenia and/or neutropenia. Some cases develop from exposure to ionizing radiation or cytotoxic chemotherapy, usually with alkylating agents, and in these circumstances the bone marrow is characteristically hypocellular and partially fibrotic
  • 16. Classification Sr. No. Disease Blood findings Bone marrow findings 1 Refractory cytopenias with unilineage dysplasia (RCUD) Uni / bi-cytopenias No or rare blasts (<1%) Unilineage dysplasia: > 10% of the cells in one myeloid lineage <5% blasts <15% of erythroid precursors are ring sideroblasts 2 Refractory anemia with ring siderblasts (RARS) Anemia No blasts >15% of erythroid precursors are ring sinderblasts Erythroid dysplasia only <5% blasts 3 Refractory cytopenia with multilineage dysplasia (RCDM) Cytopenia(s) No or rare blasts No Auer rods <1 x 109/L monocytes Dysplasia in >10% of the cells in >2 myeloid lineages <5% blasts No auer rods +/- 15% ring sideroblasts
  • 17. Sr. No. Disease Blood findings Bone marrow findings 4 Refractory Anemia with excess blasts -1 (RAEB-1) Cytopenia <5% blasts No auer rods <1 x 109/L monocytes Unilineage or multilineage dysplasia 5-9% blasts No auer rods 5 Refractory Anemia with excess blasts -2 (RAEB -2) Cytopenia 5-19% blasts +/- auer rods <1 x 109/L monocytes Unilineage or multilineage dysplasia 10-19% blasts +/- auer rods 6. Myelodysplastic syndrome – unclassified (MDS-U) Cytopenia <1% blasts Unequivocal dysplasis in ,10% cells <5% blasts 7. MDS associated with isolated del (5q) Anemia Normal to increased platelet count No or rare blasts Normal to increased megakaryocytes with hypolobated nuclei <5% blasts Isolated del(5q) No auer rods
  • 18. Fanconi’s Anemia • Autosomal recessive • FA is the result of a genetic defect in a cluster of proteins responsible for a DNA repair.
  • 19. • As a result, the majority of FA patients develop cancer, most often acute myelogenous leukemia in 33%, and 90% develop bone marrow failure by the age of 40. • Most commonly M4 (Myelomonocytic) and M5 (monocytic)
  • 20. • Significant risk of solid tumors like • Hepatic tumors • Squamous cell carcinoma • 28% calculated risk by the age 40
  • 21. Cell and Molecular Biology • FA cells characteristically display a high frequency of spontaneous chromosomal breakage and hypersensitivity to DNA cross-linking agents. • A subset of patients also present with biallelic mutations in BRCA2 gene • BRCA2 protein is important in the repair of DNA damage. • Thus, cells lacking BRCA2 inaccurately repair damaged DNA and are hypersensitive to DNA crosslinking agents.
  • 22. Signs and Symptoms • During childhood, short stature and skin pigmentation, including café au lait spots, may become apparent. • The first sign of a hematologic problem is usually petechiae and bruises, with later onset of pale appearance, feeling tired, and infections. • Somatic abnormalities such as Skeletal (absent thumbs, radial hypoplasia, scoliosis), genitourinary ( inferitility, horseshoe kidneys) , gastrointestinal, cardiac and neurological may be present
  • 24. Treatment • Administration of oxymetholone, corticosteroids can show response in upto 70% patients but many will become refractory after variable time • Hematopoietic stem cell transplant is the treatment of choice.
  • 25. Dyskeratosis Congenita • X-linked recessive, autosomal dominant and autosomal recessive forms • Bone marrow failure develops below the age of 20 years; 80-90% will develop bone marrow abnormalities by age 30 yrs.
  • 26. Cell and Molecular Biology • Peripheral blood and bone marrow metaphases from patients show unbalanced chromosomal rearrangements in the absence of any clastogenic agents • Chromosome/genomic instability • Defect in DKC1 gene leading to defective ribosome production • Hematopoietic progenitor studies have shown reduced numbers of all progenitors.
  • 27. Signs and Symptoms • Characterized by the mucocutaneous triad of abnormal skin pigmentation, nail dystrophy and mucosal leucoplakia • Bone marrow failure is the principal cause of early mortality with an early predisposition to AML • Non-cutaneous lesions such as short stature, pulmonary disease, esophageal strictures have been documented.
  • 28. Treatment • Transient successful responses to granulocyte/macrophage colony-stimulating factor, Granulocyte colony-stimulating factor and erythropoietin have been reported • Steroid oxymetholone • Hematopoietic Stem cell transplant
  • 29. Shwachman-Diamond Syndrome • Shwachman–Diamond syndrome is characterized by an autosomal recessive mode of inheritance. The gene that is mutated in this syndrome lies on the long arm of chromosome 7 at cytogenetic position 7q11 • rare congenital disorder characterized by exocrine pancreatic insufficiency, bone marrow dysfunction, skeletal abnormalities, and short stature. After cystic fibrosis (CF), it is the second most common cause of exocrine pancreatic insufficiency in children.
  • 30. Cell and Molecular biology • The SDS gene is on 7q11.22 which is mutated in 90% patients. • Its importance in indicated in RNA metabolism and ribosome biogenesis.
  • 31. Hematological abnormalities • Neutropenia - Low neutrophil counts leave patients at risk of developing severe recurrent infections that may be life-threatening. • Anemia and thrombocytopenia may also occur. Bone marrow is typically hypocellular, with maturation arrest in the myeloid lineages that give rise to neutrophils, macrophages, platelets and red blood cells. • Patients may also develop progressive marrow failure or transform to acute myelogenous leukemia.
  • 32. Treatment • G-CSF • Incidence of myelodysplasia and transformation to AML is seen in 15-25% • Particularly AML with erythroid differentiation: M6
  • 33. Blackfan-Diamond Syndrome • Most pedigrees suggest an autosomal dominant mode of inheritance with incomplete penetrance. Approximately 10–25% of DBA occurs with a family history of disease. • Inherited pure red cell aplasia is a congenital erythroid aplasia that usually presents in infancy. • DBA causes anemia, without substantially affecting the other blood
  • 34. Diagnostic criteria • Normochromic macrocytic Anemia • Reticulocytopenia • Normocellular bone marrow with selective deficiency of erythroid precursors • Decreased leukocyte counts with normal to increased platelet counts • Elevated erythrocyte deaminase activity
  • 35. Kostmann Agranulocytosis • Kostmann disease is a form of severe congenital neutropenia which is a rare autosomal recessive condition in which severe chronic neutropenia is detected soon after birth.
  • 36. Diagnosis • An absolute neutrophil count chronically less than 500/mm3, usually less than 200/mm3, is the main sign of Kostmann's. • Other elements include the severity of neutropenia, and other normal findings (hemoglobin, platelets) • Isolated neutropenia in infants can occur in viral infections, autoimmune neutropenia of infancy, bone marrow suppression from a drug or toxin, hypersplenism, and passive placental transfer of maternal IgG • The bone marrow usually shows early granulocyte precursors, but myelopoietic development stops at the promyelocyte and/or myelocyte stage, so that few maturing forms are seen.
  • 37. Bloom Syndrome • are autosomal recessive disorder characterized by short stature, caused by mutations in the BLM gene leading to mutated DNA helicase protein formation.
  • 38. Signs and Symptoms • short stature and a rash on the face • moderate immune deficiency, characterized by deficiency in certain immunoglobulin classes and apparently leading to recurrent pneumonia and ear infections. • low birth weight • Hypogonadism is characterized by a failure to produce sperm, hence infertility in males, and premature cessation of menses (premature menopause)

Notas del editor

  1. This is in contrast to Shwachman–Bodian–Diamond syndrome, in which the bone marrow defect results primarily in neutropenia, and Fanconi anemia, where all cell lines are affected resulting in pancytopenia