Acute lymphoblastic leukemia

Changed by Rohit Sharma, 19 Feb 2023
Disclosures - updated 17 Aug 2022: Nothing to disclose

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Acute lymphoblastic leukaemia (ALL) is a malignant disorder of the bone marrow characterised by the proliferation of the lymphoid progenitor cells, typically of the B cell lineage.

Epidemiology

Acute lymphoblastic leukaemia is the commonest form of childhood leukaemia, accounting for ~80% of paediatric leukaemia cases 1. In adults, ALL corresponds to ~20% of leukaemia cases 1. Peak age is between 3 to 7 years, with a second peak over 40 years.

Clinical presentation

The clinical features of acute lymphoblastic leukaemia are non-specific. Children commonly have at least one pallor, fever, a palpable liver, a palpable spleen, or bruising on diagnosis 2. Other symptoms such as bone or joint pain, weight loss, anorexia, bleeding, abdominal pain and abdominal distension are also common.

Pathology

In acute lymphoblastic leukaemia, the lymphoid progenitor cells, also known as lymphoblasts, do not mature due to abnormal expression of genes, often as a result of chromosomal abnormalities or chromosomal translocations (e.g. BCR/ABL1). The proliferation of the primitive cells takes up more and more marrow space at the expense of the normal haematopoietic elements, resulting in a decrease in the production of normal blood cells and bone marrow failure. Eventually, the lymphoblasts spill into the blood and can affect the liver, spleen, central nervous system, and lymph nodes.

Radiographic features

Plain radiograph

Bone lesions are common in leukaemia. A metaphyseal radiolucent band is one of the most important radiological findings 3. Other radiological findings include subperiosteal new bone formation and osteolytic lesions involving the medullary cavity and cortex 1,3-5.

Chest radiographs may reveal a mediastinal mass.

Treatment and prognosis

The treatment for acute lymphoblastic leukaemia typically has three phases:

  • induction therapy: combination chemotherapy is used to rapidly kill tumour cells to get the patient into remission

  • consolidation phase: if remission is achieved, further chemotherapy is given during this phase to treat the residual disease

  • maintenance phase: if the patient is still in remission after the consolidation phase, maintenance oral therapy is given

    • this may last up to three years if the patient remains in remission

A new novel approach replacing chemotherapeutic regimes with dasatinibThe exact treatment regimens used in managing ALL are beyond the scope of this article, blinatumomab but depend on factors such as whether the disease is B or T cell ALL, and dexamethasone has shown promising and disease-free survival outcomes 8whether positive or negative for BCR-ABL1 mutation.

Paediatric patients with acute lymphoblastic leukaemia have an overall five-year survival rate of 80% depending on their risk profile 6. However, only 30-40% of adults with ALL achieve long-term remission with the current treatment regimens 7.

Differential diagnosis

For acute lymphoblastic leukaemia bony abnormalities, consider: 

  • -<p><strong>Acute lymphoblastic leukaemia (ALL)</strong> is a malignant disorder of the <a href="/articles/bone-marrow">bone marrow</a> characterised by the proliferation of the lymphoid progenitor cells.</p><h4>Epidemiology</h4><p>Acute lymphoblastic leukaemia is the commonest form of childhood <a href="/articles/leukaemia">leukaemia</a>, accounting for ~80% of paediatric leukaemia cases <sup>1</sup>. In adults, ALL corresponds to ~20% of leukaemia cases <sup>1</sup>. Peak age is between 3 to 7 years, with a second peak over 40 years.</p><h4>Clinical presentation</h4><p>The clinical features of acute lymphoblastic leukaemia are non-specific. Children commonly have at least one pallor, <a href="/articles/pyrexia">fever</a>, <a href="/articles/hepatomegaly">a palpable liver</a>, <a href="/articles/splenomegaly">a palpable spleen</a>, or bruising on diagnosis <sup>2</sup>. Other symptoms such as bone or joint pain, <a href="/articles/weight-loss">weight loss</a>, anorexia, bleeding, abdominal pain and abdominal distension are also common.</p><h4>Pathology</h4><p>In acute lymphoblastic leukaemia, the lymphoid progenitor cells, also known as lymphoblasts, do not mature due to abnormal expression of genes, often as a result of chromosomal abnormalities or chromosomal translocations. The proliferation of the primitive cells takes up more and more marrow space at the expense of the normal haematopoietic elements, resulting in a decrease in the production of normal blood cells and bone marrow failure. Eventually, the lymphoblasts spill into the blood and can affect the <a href="/articles/liver">liver</a>, <a href="/articles/spleen-1">spleen</a>, central nervous system, and lymph nodes.</p><h4>Radiographic features</h4><h5>Plain radiograph</h5><p>Bone lesions are common in leukaemia. A <a href="/articles/lucent-transverse-metaphyseal-lines-mnemonic">metaphyseal radiolucent band</a> is one of the most important radiological findings <sup>3</sup>. Other radiological findings include subperiosteal new bone formation and osteolytic lesions involving the medullary cavity and cortex <sup>1,3-5</sup>.</p><p>Chest radiographs may reveal a <a href="/articles/mediastinal-mass">mediastinal mass</a>.</p><h4>Treatment and prognosis</h4><p>The treatment for acute lymphoblastic leukaemia typically has three phases:</p><ul>
  • -<li>induction therapy: combination chemotherapy is used to rapidly kill tumour cells to get the patient into remission</li>
  • -<li>consolidation phase: if remission is achieved, further chemotherapy is given during this phase to treat the residual disease</li>
  • -<li>maintenance phase: if the patient is still in remission after the consolidation phase, maintenance oral therapy is given<ul><li>this may last up to three years if the patient remains in remission</li></ul>
  • +<p><strong>Acute lymphoblastic leukaemia (ALL)</strong> is a malignant disorder of the <a href="/articles/bone-marrow">bone marrow</a> characterised by the proliferation of the lymphoid progenitor cells, typically of the B cell lineage.</p><h4>Epidemiology</h4><p>Acute lymphoblastic leukaemia is the commonest form of childhood <a href="/articles/leukaemia">leukaemia</a>, accounting for ~80% of paediatric leukaemia cases <sup>1</sup>. In adults, ALL corresponds to ~20% of leukaemia cases <sup>1</sup>. Peak age is between 3 to 7 years, with a second peak over 40 years.</p><h4>Clinical presentation</h4><p>The clinical features of acute lymphoblastic leukaemia are non-specific. Children commonly have at least one pallor, <a href="/articles/pyrexia">fever</a>, <a href="/articles/hepatomegaly">a palpable liver</a>, <a href="/articles/splenomegaly">a palpable spleen</a>, or bruising on diagnosis <sup>2</sup>. Other symptoms such as bone or joint pain, <a href="/articles/weight-loss">weight loss</a>, anorexia, bleeding, abdominal pain and abdominal distension are also common.</p><h4>Pathology</h4><p>In acute lymphoblastic leukaemia, the lymphoid progenitor cells, also known as lymphoblasts, do not mature due to abnormal expression of genes, often as a result of chromosomal abnormalities or chromosomal translocations (e.g. <em>BCR/ABL1</em>). The proliferation of the primitive cells takes up more and more marrow space at the expense of the normal haematopoietic elements, resulting in a decrease in the production of normal blood cells and bone marrow failure. Eventually, the lymphoblasts spill into the blood and can affect the <a href="/articles/liver">liver</a>, <a href="/articles/spleen-1">spleen</a>, central nervous system, and lymph nodes.</p><h4>Radiographic features</h4><h5>Plain radiograph</h5><p>Bone lesions are common in leukaemia. A <a href="/articles/lucent-transverse-metaphyseal-lines-mnemonic">metaphyseal radiolucent band</a> is one of the most important radiological findings <sup>3</sup>. Other radiological findings include subperiosteal new bone formation and osteolytic lesions involving the medullary cavity and cortex <sup>1,3-5</sup>.</p><p>Chest radiographs may reveal a <a href="/articles/mediastinal-mass">mediastinal mass</a>.</p><h4>Treatment and prognosis</h4><p>The treatment for acute lymphoblastic leukaemia typically has three phases:</p><ul>
  • +<li><p>induction therapy: combination chemotherapy is used to rapidly kill tumour cells to get the patient into remission</p></li>
  • +<li><p>consolidation phase: if remission is achieved, further chemotherapy is given during this phase to treat the residual disease</p></li>
  • +<li>
  • +<p>maintenance phase: if the patient is still in remission after the consolidation phase, maintenance oral therapy is given</p>
  • +<ul><li><p>this may last up to three years if the patient remains in remission</p></li></ul>
  • -</ul><p>A new novel approach replacing chemotherapeutic regimes with dasatinib, blinatumomab and dexamethasone has shown promising and disease-free survival outcomes <sup>8</sup>.</p><p>Paediatric patients with acute lymphoblastic leukaemia have an overall five-year survival rate of 80% depending on their risk profile <sup>6</sup>. However, only 30-40% of adults with ALL achieve long-term remission with the current treatment regimens <sup>7</sup>.</p><h4>Differential diagnosis</h4><p>For acute lymphoblastic leukaemia bony abnormalities, consider: </p><ul>
  • -<li><a href="/articles/juvenile-idiopathic-arthritis">juvenile idiopathic arthritis</a></li>
  • -<li><a href="/articles/osteomyelitis">osteomyelitis</a></li>
  • -<li><a href="/articles/aplastic-anaemia">aplastic anaemia</a></li>
  • -<li><a href="/articles/acute-infectious-lymphocytosis">acute infectious lymphocytosis</a></li>
  • +</ul><p>The exact treatment regimens used in managing ALL are beyond the scope of this article, but depend on factors such as whether the disease is B or T cell ALL, and whether positive or negative for <em>BCR-ABL1</em> mutation.</p><p>Paediatric patients with acute lymphoblastic leukaemia have an overall five-year survival rate of 80% depending on their risk profile <sup>6</sup>. However, only 30-40% of adults with ALL achieve long-term remission with the current treatment regimens <sup>7</sup>.</p><h4>Differential diagnosis</h4><p>For acute lymphoblastic leukaemia bony abnormalities, consider: </p><ul>
  • +<li><p><a href="/articles/juvenile-idiopathic-arthritis">juvenile idiopathic arthritis</a></p></li>
  • +<li><p><a href="/articles/osteomyelitis">osteomyelitis</a></p></li>
  • +<li><p><a href="/articles/aplastic-anaemia">aplastic anaemia</a></p></li>
  • +<li><p><a href="/articles/acute-infectious-lymphocytosis">acute infectious lymphocytosis</a></p></li>

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