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Course Outline
 1. Introduction
 2. Definition of leukemia
 3. Etiology
 4. Epidemiology of childhood acute lymphoblastic leukemia
 5. Clinical presentation
 6. Diagnosis
 7. Management
 8. Complications
 9. Prognosis
 10. Prevention
Introduction
Leukemia is a type of cancer of blood or bone marrow characterized by proliferation of
immature white cells,
Acute lymphoblastic leukemia (ALL) is a malignancy of B or T lymphoblasts characterized
by uncontrolled proliferation of abnormal, immature lymphocytes and their progenitors
which ultimately leads to the replacement of bone marrow elements and other lymphoid
organs resulting in a typical disease pattern characteristic of Acute Lymphocytic Leukemia
is the commonest pediatric malignant.
ALL is fourfold compared to AML, and account 80 % of childhood.
It occurs in male than in female and more common in white than in black.
Clinical manifestation is related to ; anemia, thrombocytopenia, neutropenia and CNC
manifestation.
Epidemiology
 Most common malignant of childhood.
 4000 people/year of patient under 18 year is diagnosed in USA.
 It occurs more in children of Trisomy 21, neurofipromatosis 1, ataxia telangiectasia.
 Peak age :2-10 years, but more common between 2-3 years .
 Poor prognosis in children under 1 year and adult people.
 It’s survival rate is increasing greater than 85% in last five years.
Etiology
 Etiology of Acute Lymphoblastic Leukemia is unknown.
 Some suggest environmental factors such as: exposure to benzene, ionizing radiation
and exposure to previous radiotherapy or chemotherapy.
 It is not familial related.
 Certain genomic particularly p53.
Clinical presentation
 ALL clinical presentation mainly related with diminished in blood components.
 In history of patient:
 Anemia: weakness, dizziness, musculoskeletal pain.
 Neutropenia: fever occurred due to infection
 Thrombocytopenia: easily bleeding ( epistaxis, gingival bleeding etc..)
 Mainly has B-symptoms ( constitutional symptoms) : fever, night sweat, weight loss.
Clinical presentation
 On physical examination:
 Hepatomegaly and splenomegaly( 64%, 61%)
 Easily bruising
 Joint tenderness
 Central or peripheral pallor
 Lymphadenopathy which may be identified in history or on P/E
Cont’
 Some symptoms implicated to involvement of CNS such as headache, lethargy,
nuchal rigidity, vomiting
 Testicular enlargement with up to 10 % is due to relapsed leukemia
 Mediastinal mass which can cause Superior Vena Cava Syndrome (dysphagia,
dyspnea, or swelling of the neck, face, and upper limbs )
Diagnosis
 ALL is diagnosed based on clinical presentation and laboratories, imaging modalities, if
you suspect leukemia you have to transfer to pediatric oncology for evaluation,
diagnosis and management.
 Testing for: Complete morphologic, Immunophenotypic characterization, genetic and
leukemic cells
 Laboratories: CBC, electrolytes and renal panel, LDH level.
 If patient has respiratory symptoms do chest x-ray
Diagnosis cont’
 If has abdominal tenderness do CT-scan of abdomen and pelvis.
 Lumbar puncture for CSF ( presence of lymphoblasts) analysis if CNS involvement.
 Do bone marrow, lymph node aspiration and biopsy for histopathology study.
 Cytochemistry ( Periodic Acid Schiff, Nonspecific Esterase, Myeloperoxidase) for
classification
Management of ALL
 Before treatment of ALL, you should evaluate:
 Laboratories such as :- Chemistry ( Electrolytes, liver and renal function test, LDH, uric acid ,
calcium and phosphate)
- Coagulation profiles ( Prothrombin time, partial prothrombin time, fibrinogen)
 Lumbar puncture/Neurological evaluation: before ALL treatment you do lumbar puncture for
evaluation of potential leukemic involvement of CNS inorder to give prophylactic first dose of intrathecal
therapy.
1. CNS-1: no lymphoblasts in CSF regardless of WBC
2. CNS-2: <5 WBC/micro in CSF with presence of lymphoblasts
3. CNS-3: > or = 5 WBC/micro in CSF with presence of lymphoblasts
Management cont’
 Other pretreatment evaluation includes:
 Screen for infection and initiate empirical treatment appropriately
 Cardiac evaluation with Echocardiogram ( anticipation of Anthracycline)
 Human leucocyte Antigen (HLA) typing during hematopoietic stem cell transplant.
 CT scan of chest to evaluate mediastinal mass
Management cont’
 Management of child with leukemia as for every cancer is multidisciplinary.
 You have to transfer to pediatric cancer specialist or center for better follow up and
management.
 Treatment of ALL has Three phases:
o Remission-Induction phase ,therapy with mainly corticosteroids, anthracycrine,
vincristine and 1- asparginase
o Intensification/Consolidation therapy widely used and include variety of
chemotherapeutic drugs with good outcomes( cyclophosphamide cytarabine,
dexamethasone, MTX etc…).
Management cont’
o Maintenance therapy uses oral 6-mercaptopurine or methotrexate once a week or once a
month.
 Additional the drugs directed to CNS consists of systemic chemotherapy that enters the
CSF as well as intrathecal MTX for entire course of treatment
Management cont’
 The treatment last in between 2-3 years to be completed.
 Patient may undergo splenectomy for boosting platelets count but does not affect the
outcome, also radiotherapy is used for reduce splenomegaly.
 Patient can be undergo transfusion of all required blood products.
 In cancer center they sometime use medication related to type of ALL.
 You treat infection accordingly based on culture result.
 As for those children has malnutrition, require nutritional support.
Complications
 Some complications are related to the treatments others due to ALL
1. Tumor lysis syndrome the life threatening complication related to chemotherapy
and characterized with:
 Hyperuricemia
 Hyperkalemia
 Hyperphosphatemia and
 Hypocalcaemia
2. Renal failure which is invariable
Complication cont’
 Luekostasis which is oncologic emergency also TLS,
It may manifest due to stasis of leukocyte in different organs:
1. Respiratory: dyspnea, hypoxemia, respiratory failure
2. Nuerologic involvement : somnolence, coma or focal neurologic deficit
Complication cont’
3. Sepsis
4. Bleeding
5. Seizures
6. Encephalopathy
7. Thrombosis
8. Cognitive defects
9. Secondary malignancy
Prognosis
 The likelihood of long-term cure in ALL depends on the clinical and laboratory features
and the treatment.
o Prognostic risk assessment :
1. Age
2. WBC count
3. Complete remission within 4 weeks
4. Cytogenetics
Prognosis cont’
 Classification of prognosis based on criteria :
1. Low risk
2. Average or standard risk: age of 1-9.9 years, WBC count less than 50,000 at
presentation, good response to initial treatment, lack of cytogenetic features
3. High risk
4. Very high risk
Prevention
 Prevention is based on prevention of environmental risk factors
Which stated in etiology
References:
1. www.uptodate.com
2. www.medscape.com
3. Acute lymphocytic leukemia article by Yana Puckett, Onyee Chan
Thank
Your inputs are welcome

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Childhood acute lympocytic leukemia

  • 1. Course Outline  1. Introduction  2. Definition of leukemia  3. Etiology  4. Epidemiology of childhood acute lymphoblastic leukemia  5. Clinical presentation  6. Diagnosis  7. Management  8. Complications  9. Prognosis  10. Prevention
  • 2. Introduction Leukemia is a type of cancer of blood or bone marrow characterized by proliferation of immature white cells, Acute lymphoblastic leukemia (ALL) is a malignancy of B or T lymphoblasts characterized by uncontrolled proliferation of abnormal, immature lymphocytes and their progenitors which ultimately leads to the replacement of bone marrow elements and other lymphoid organs resulting in a typical disease pattern characteristic of Acute Lymphocytic Leukemia is the commonest pediatric malignant. ALL is fourfold compared to AML, and account 80 % of childhood. It occurs in male than in female and more common in white than in black. Clinical manifestation is related to ; anemia, thrombocytopenia, neutropenia and CNC manifestation.
  • 3. Epidemiology  Most common malignant of childhood.  4000 people/year of patient under 18 year is diagnosed in USA.  It occurs more in children of Trisomy 21, neurofipromatosis 1, ataxia telangiectasia.  Peak age :2-10 years, but more common between 2-3 years .  Poor prognosis in children under 1 year and adult people.  It’s survival rate is increasing greater than 85% in last five years.
  • 4. Etiology  Etiology of Acute Lymphoblastic Leukemia is unknown.  Some suggest environmental factors such as: exposure to benzene, ionizing radiation and exposure to previous radiotherapy or chemotherapy.  It is not familial related.  Certain genomic particularly p53.
  • 5. Clinical presentation  ALL clinical presentation mainly related with diminished in blood components.  In history of patient:  Anemia: weakness, dizziness, musculoskeletal pain.  Neutropenia: fever occurred due to infection  Thrombocytopenia: easily bleeding ( epistaxis, gingival bleeding etc..)  Mainly has B-symptoms ( constitutional symptoms) : fever, night sweat, weight loss.
  • 6. Clinical presentation  On physical examination:  Hepatomegaly and splenomegaly( 64%, 61%)  Easily bruising  Joint tenderness  Central or peripheral pallor  Lymphadenopathy which may be identified in history or on P/E
  • 7. Cont’  Some symptoms implicated to involvement of CNS such as headache, lethargy, nuchal rigidity, vomiting  Testicular enlargement with up to 10 % is due to relapsed leukemia  Mediastinal mass which can cause Superior Vena Cava Syndrome (dysphagia, dyspnea, or swelling of the neck, face, and upper limbs )
  • 8. Diagnosis  ALL is diagnosed based on clinical presentation and laboratories, imaging modalities, if you suspect leukemia you have to transfer to pediatric oncology for evaluation, diagnosis and management.  Testing for: Complete morphologic, Immunophenotypic characterization, genetic and leukemic cells  Laboratories: CBC, electrolytes and renal panel, LDH level.  If patient has respiratory symptoms do chest x-ray
  • 9. Diagnosis cont’  If has abdominal tenderness do CT-scan of abdomen and pelvis.  Lumbar puncture for CSF ( presence of lymphoblasts) analysis if CNS involvement.  Do bone marrow, lymph node aspiration and biopsy for histopathology study.  Cytochemistry ( Periodic Acid Schiff, Nonspecific Esterase, Myeloperoxidase) for classification
  • 10. Management of ALL  Before treatment of ALL, you should evaluate:  Laboratories such as :- Chemistry ( Electrolytes, liver and renal function test, LDH, uric acid , calcium and phosphate) - Coagulation profiles ( Prothrombin time, partial prothrombin time, fibrinogen)  Lumbar puncture/Neurological evaluation: before ALL treatment you do lumbar puncture for evaluation of potential leukemic involvement of CNS inorder to give prophylactic first dose of intrathecal therapy. 1. CNS-1: no lymphoblasts in CSF regardless of WBC 2. CNS-2: <5 WBC/micro in CSF with presence of lymphoblasts 3. CNS-3: > or = 5 WBC/micro in CSF with presence of lymphoblasts
  • 11. Management cont’  Other pretreatment evaluation includes:  Screen for infection and initiate empirical treatment appropriately  Cardiac evaluation with Echocardiogram ( anticipation of Anthracycline)  Human leucocyte Antigen (HLA) typing during hematopoietic stem cell transplant.  CT scan of chest to evaluate mediastinal mass
  • 12. Management cont’  Management of child with leukemia as for every cancer is multidisciplinary.  You have to transfer to pediatric cancer specialist or center for better follow up and management.  Treatment of ALL has Three phases: o Remission-Induction phase ,therapy with mainly corticosteroids, anthracycrine, vincristine and 1- asparginase o Intensification/Consolidation therapy widely used and include variety of chemotherapeutic drugs with good outcomes( cyclophosphamide cytarabine, dexamethasone, MTX etc…).
  • 13. Management cont’ o Maintenance therapy uses oral 6-mercaptopurine or methotrexate once a week or once a month.  Additional the drugs directed to CNS consists of systemic chemotherapy that enters the CSF as well as intrathecal MTX for entire course of treatment
  • 14. Management cont’  The treatment last in between 2-3 years to be completed.  Patient may undergo splenectomy for boosting platelets count but does not affect the outcome, also radiotherapy is used for reduce splenomegaly.  Patient can be undergo transfusion of all required blood products.  In cancer center they sometime use medication related to type of ALL.  You treat infection accordingly based on culture result.  As for those children has malnutrition, require nutritional support.
  • 15. Complications  Some complications are related to the treatments others due to ALL 1. Tumor lysis syndrome the life threatening complication related to chemotherapy and characterized with:  Hyperuricemia  Hyperkalemia  Hyperphosphatemia and  Hypocalcaemia 2. Renal failure which is invariable
  • 16. Complication cont’  Luekostasis which is oncologic emergency also TLS, It may manifest due to stasis of leukocyte in different organs: 1. Respiratory: dyspnea, hypoxemia, respiratory failure 2. Nuerologic involvement : somnolence, coma or focal neurologic deficit
  • 17. Complication cont’ 3. Sepsis 4. Bleeding 5. Seizures 6. Encephalopathy 7. Thrombosis 8. Cognitive defects 9. Secondary malignancy
  • 18. Prognosis  The likelihood of long-term cure in ALL depends on the clinical and laboratory features and the treatment. o Prognostic risk assessment : 1. Age 2. WBC count 3. Complete remission within 4 weeks 4. Cytogenetics
  • 19. Prognosis cont’  Classification of prognosis based on criteria : 1. Low risk 2. Average or standard risk: age of 1-9.9 years, WBC count less than 50,000 at presentation, good response to initial treatment, lack of cytogenetic features 3. High risk 4. Very high risk
  • 20. Prevention  Prevention is based on prevention of environmental risk factors Which stated in etiology
  • 21. References: 1. www.uptodate.com 2. www.medscape.com 3. Acute lymphocytic leukemia article by Yana Puckett, Onyee Chan