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[[The flow cytometric diagnosis of AML|--]]
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<span style="font-size:110%; color:navy">'''SECTION 1: Establishing the primitive nature of the blast cells in AML'''</span>
<span style="font-size:110%; color:navy">'''SECTION 1: Establishing the primitive nature of the blast cells in AML'''</span>


[[Image:Mac1.png|150px]]   
[[Image:AML M1.png|130px]]   


''Blast cells are recognised by morphology using features such as primitive nuclear or basophilic cytoplasmic appearances; similar principles are applied in flow cytometry where particular markers suggest a more primitive nature.
''Blast cells are recognised by morphology using features such as primitive nuclear or basophilic cytoplasmic appearances; similar principles are applied in flow cytometry where particular markers suggest a more primitive nature.
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<div style="width: 95%">
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{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" data-expandtext="Click to open Table" data-collapsetext="Click to close table"
{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" </br>data-expandtext="Click to open Table" data-collapsetext="Click to close table"
! colspan="2" style = "font-size:100%; color:black"| '''Table:''' Markers primarily used to confirm primitive nature in AML. &nbsp;
! colspan="2" style = "font-size:100%; color:black"| '''Table:''' Markers primarily used to confirm primitive nature in AML. &nbsp;
|-  
|-  
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1"|The expression of some markers is typically associated with primitive cells and can help recognise the primitive nature of blast cells.
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1"|The expression of some markers is typically associated with primitive cells and can help recognise the primitive nature of blast cells.</br>Note that these markers may also have some lineage specificity but are not generally used to assign lineage
 
Note that these markers may also have some lineage specificity but are not generally used to assign lineage
|-
|-
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD45]]'''
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD45]]'''
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|colspan="1" style = "font-size:90%;"|Frequently expressed by AML blast cells (40-80% of cases) - most often in less differentiated forms of AML. Expression is also seen frequently (and often more strongly) in ALL'''
|colspan="1" style = "font-size:90%;"|Frequently expressed by AML blast cells (40-80% of cases) - most often in less differentiated forms of AML. Expression is also seen frequently (and often more strongly) in ALL'''
|-
|-
|colspan="2" style = "font-size:90%; color:black; background:light gray" |'''Other markers:''' In the context of a proven AML diagnosis a number of markers may be expressed that reflect the primitive nature of the cells. Some of these are more frequently associated with lymphoid disorders, but providing other criteria for AML are met they should simply be considered to show "primitivness".  
|colspan="2" style = "font-size:90%; color:black; background:light gray" |'''Other markers:''' In the context of a proven AML diagnosis a number of markers may be expressed that reflect the primitive nature of the cells. Some of these are more frequently associated with lymphoid disorders, but providing other criteria for AML are met they should simply be considered to show "primitivness".</br>These include: [[CD38]], [[HLA-DR]], [[TDT]], [[CD7]].
 
These include: [[CD38]], [[HLA-DR]], [[TDT]], [[CD7]].
|-
|-
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<span style="font-size:110%; color:navy">'''SECTION 2: Assigning blast cells as myeloid lineage'''</span>
<span style="font-size:110%; color:navy">'''SECTION 2: Assigning blast cells as myeloid lineage i.e. Diagnosing AML'''</span>


[[Image:Mac1.png|150px]]   
[[Image:AML M2.png|150px]]   


''In morphology other features are used to indicate myeloid lineage, some are highly specificsuch as Auer rods, others may suggest myeloid lineage but be less specific. Again similar principles apply in flow cytometry''
''In morphology other features are used to indicate myeloid lineage, some are highly specificsuch as Auer rods, others may suggest myeloid lineage but be less specific. Again similar principles apply in flow cytometry''
 
 
There are two ways to assign myeloid lineage in AML:
 
'''1. ''' Myeloid can be assigned if '''a simgle lineage-defining''' marker is expressed. If there are no lineage-defining features of B or T-lineage then the diagnosis is AML (Table 1). If there are B or T lineage markers also present consider whether the criteria are met to diagnose a mixed phenotype acute leukaemia [[MPAL]]
 
'''2.''' Alternatively myeloid can be assigned if '''at least two myeloid-associated markers''' are expressed, provinding lineage cannot be assigned as B cell or T cell by lineage-specific, or by lineage-associated lymphoid markers (Table 2A and 2B). If there is significant expression of lymphoid lineage markers consider whether criteria for [[MPAL]] are met.




There are two ways to make a diagnosis of AML
<div style="width: 95%"; >
{| class="wikitable"
!colspan="2" style = "background:lightgrey; border:solid"| '''Requirements to diagnose AML by flow cytometry'''
|-
!colspan="1" style = "background:#FFFFF0;border:solid; font-size:90%;"| '''Pattern 1:'''</br>A myeloid '''lineage-defining''' marker pattern is present</br>'''and'''</br>No lineage-defining markers of T or B cells are present
!colspan="1" style = "background:white; border:solid; font-size:90%;"|See '''[[#AML_Table1|Table 1]]''' for lineage-defining marker patterns in AML
|-
!colspan="1" style = "background:#FFFFF0;border:solid; font-size:90%;"|'''Pattern 2''':</br>At least '''two myeloid lineage-associated''' markers are present</br>'''and'''</br>There are no lineage defining markers of T or B cells</br>'''and'''</br>No more than one: T-cell '''or''' B-cell lineage-associated markers are  present
!colspan="1" style = "background:white; border:solid; font-size:90%;"|See '''[[#AML_Table2A|Table 2A]]''' and '''[[#AML_Table2B|Table 2B]]''' for lineage-associated markers in AML
|}
</div>
----
<div id="AML_Table1">'''Table 1'''</div>
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{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" data-expandtext="Click to open Table" data-collapsetext="Click to close table"
{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" data-expandtext="Click to open Table" data-collapsetext="Click to close table"
!colspan="2" <span style="font-size:100%; colour:white; text-align:left; border: 1px solid black; background:pale gray">|'''Table 1:''' Myeloid-lineage defining markers in AML </span><span style="font-size:100%; text-align:left; background:white">
!colspan="2" <span style="font-size:100%; colour:white; text-align:left; border: 1px solid black; background:pale gray">|Myeloid-lineage defining markers in AML </span><span style="font-size:100%; text-align:left; background:white">
|-  
|-  
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1"|Only one marker is presently used to assign myeloid lineage in AML (note restrictions)
|colspan="2" <span style = "font-size:90%; color:black; background:#ddeee1">|Lineage is defined by either the definite assignment to myeloid lineage or definite assignment to monocytic lineage. In each case there are specific criteria.
 
|-
Note that these markers may also have some lineage specificity but are not generally used to assign lineage
|colspan="1" style = "font-size:90%; color:black;" |'''Myeloperoxidase''' is expressed
|colspan="1" style = "font-size:90%;"|[[MPO]] is lineage-defining in AML (expressed in around 80% of cases)
|-
|-
|colspan="1" style = "font-size:100%; color:black;" |'''[[MPO]]'''
|colspan="1" style = "font-size:90%; color:black;" |'''Monocytic lineage''' can be assigned.
|colspan="1" style = "font-size:100%;"|A '''lineage-defining''' marker in AML when expressed (around 80% of cases). More frequent in cases with granulocytic maturation. When detected by flow cytometry is diagnostic of myeloid differentiation is established (either AML or MPAL)
|colspan="1" style = "font-size:90%;"|This requires detection of at least two of: [[CD14]], [[CD11c]], [[CD64]], [[NSE]], lysozyme*
|}
|}
</div>
</div>
----
<div id="AML_Table2A">'''Table 2A'''</div>
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{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" data-expandtext="Click to open Table" data-collapsetext="Click to close table"
!colspan="2" <span style="font-size:100%; colour:white; text-align:left; border: 1px solid black; background:pale gray">|'''Table 2A:''' Myeloid lineage-associated markers (Main Set)'''</span><span style="font-size:90%; text-align:left; background:white">
!colspan="2" <span style="font-size:100%; colour:white; text-align:left; border: 1px solid black; background:pale gray">|Myeloid lineage-associated markers (Main Set)'''</span><span style="font-size:90%; text-align:left; background:white">
|-
|-
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1" |Each of these markers is frequently expressed in AML (80% of cases). They support a diagnosis of myeloid lineage, but are not sufficiently specific to be AML-defining when expressed alone
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1" |Each of these markers is supports a diagnosis of myeloid lineage, but are not AML-defining when expressed alone. However, in the absence of markers suggesting alternative lineage expression of '''two''' of these markers may be used to assign myeloid lineage.
<span style="font-size:90%;></br>These markers may be considered the most frequent markers expressed by AML. Having said that each may also be expressed by cells of ALL. General concepts:
* In the absence of markers suggesting alternative lineage expression of two of these markers may be used to support a diagnosis of AML
* One or more of CD117, CD33, CD13 may be expressed by otherwise typical ALL is allowed and does not change lineage assignment
</br>
</br>
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<div id="AML_Table2B">'''Table 2B'''</div>
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{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" data-expandtext="Click to open Table" data-collapsetext="Click to close table"
{| class="mw-collapsible mw-collapsed wikitable" style="border-style: solid; border-width: 5px; color:black" data-expandtext="Click to open Table" data-collapsetext="Click to close table"
!colspan="2" <span style="font-size:100%; colour:white; text-align:left; border: 1px solid black; background:pale gray">|'''Table 2B:''' Myeloid lineage-associated markers (Specific differentiation)'''</span><span style="font-size:90%; text-align:left; background:white">
!colspan="2" <span style="font-size:100%; colour:white; text-align:left; border: 1px solid black; background:pale gray">|Myeloid lineage-associated markers (Specific differentiation)'''</span><span style="font-size:90%; text-align:left; background:white">
|-
|-
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1" |The markers already decribed are sufficient to make a diagnosis of typical AML in most cases. Typically the markers in this table are associated with specific features of differentiation so will not be present in all cases, but may be helpful as "lineage-assocated" markers in difficult cases. Care should be taken when doing so, since in some cases specificity may be lower than for typical myeloid markers.  
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1" |The markers already described above are sufficient to make a diagnosis of typical AML in most cases. Typically the markers in this table are associated with specific features of differentiation so will not be present in all cases, but may be helpful as "lineage-assocated" markers in difficult cases. Care should be taken when doing so, since in some cases specificity may be lower than for typical myeloid markers.  
|-
|-
!colspan="2" style = "font-size:90%;background:white;"|Granulocytic lineage markers
!colspan="2" style = "font-size:90%;background:white;"|Additional features of granulocytic maturation
|-
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD10]]'''
|colspan="1" style = "font-size:84%;"|Most frequently a marker expressed in ALL subtypes, but expression of CD10 may occur some more differentiated cases of AML (particularly APL and AML with monocytic maturation  
|-
|-
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD11b]]'''
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD11b]]'''
|colspan="1" style = "font-size:84%;"|A marker of both granulocytic and monocytic maturation, this marker has previously been associated with less good outcome in a number of studies
|colspan="1" style = "font-size:84%;"|A marker of both granulocytic and monocytic maturation, this marker has previously been associated with less good outcome in a number of studies
|-
|-
!colspan="2" style = "font-size:90%;background:white;"|Monocytic lineage markers
!colspan="2" style = "font-size:90%;background:white;"|Addtional features of monocytic differentiation
|-
|-
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD11c]]'''
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD11c]]'''
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|colspan="1" style = "font-size:84%;"|A good lineage marker for monocytic differentiation in AML, expressed in both monoblastic and monocytic forms, not fully sepicific when expressed at lower levels.
|colspan="1" style = "font-size:84%;"|A good lineage marker for monocytic differentiation in AML, expressed in both monoblastic and monocytic forms, not fully sepicific when expressed at lower levels.
|-
|-
!colspan="2" style = "font-size:90%;background:white;"|'''Features associated with erythroid differentiation'''
!colspan="2" style = "font-size:90%;background:white;"|Features associated with erythroid differentiation
|-
|-
|colspan="2" style = "font-size:90%;background:white;"|Most often [[CD34]], [[CD45]] and [[HLA-DR]] are weak or negative, although [[CD117]] and [[CD36]] are generally expressed. There may be some expression of platelet markers in some cases.
|colspan="2" style = "font-size:90%;background:white;"|Most often [[CD34]], [[CD45]] and [[HLA-DR]] are weak or negative, although [[CD117]] and [[CD36]] are generally expressed. There may be some expression of platelet markers in some cases.
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|colspan="1" style = "font-size:84%;"|A good marker of erythroid differentiation but acquired late and therefore may not be expressed
|colspan="1" style = "font-size:84%;"|A good marker of erythroid differentiation but acquired late and therefore may not be expressed
|-
|-
!colspan="2" style = "font-size:90%;background:white;"|'''Features associated with megakaryocytic differentiation'''
!colspan="2" style = "font-size:90%;background:white;"|Features associated with megakaryocytic differentiation
|-
|-
|colspan="2" style = "font-size:90%;background:white;"|Most often [[CD34]], [[CD45]] and [[HLA-DR]] are weak or negative, although [[CD13]] and [[CD33]] may be expressed
|colspan="2" style = "font-size:90%;background:white;"|Most often [[CD34]], [[CD45]] and [[HLA-DR]] are weak or negative, although [[CD13]] and [[CD33]] may be expressed
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|colspan="1" style = "font-size:90%; color:black;" |'''[[CD61]]'''
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD61]]'''
|colspan="1" style = "font-size:84%;"|Platelet glycoprotein IIIa
|colspan="1" style = "font-size:84%;"|Platelet glycoprotein IIIa
|-
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD42b]]'''
|colspan="1" style = "font-size:84%;"|Platelet gycoprotein Ib
|-
|-
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD36]]'''
|colspan="1" style = "font-size:90%; color:black;" |'''[[CD36]]'''
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<span style="font-size:110%; color:navy">'''SECTION 3: When to consider alternative lineage assignment'''</span>
<span style="font-size:110%; color:navy">'''SECTION 3: When to consider alternative lineage assignment'''</span>


The "aberrent" expression of lymphoid markers is frequently encountered in AML, and in some diagnoses their presence may be expected. The interpretation of these markers will very much depennd on the nature of the marker and/or the number of aberent markers detected. A broad guide to interpretation is given in Table 3 below.
The "aberrent" expression of lymphoid markers is frequently encountered in AML (and in some patterns of mutation these may be expected); however when non-myeloid markers are found it is important to consder if this changes lineage assignment. There are several conditions that should be considered:




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{| class="mw-collapsible mw-collapsed wikitable" style="border-style: none; border-width: 0px; colour:background:pale blue; color:black" data-expandtext="Click for details" data-collapsetext="Click to close section"
{| class="wikitable"  
!colspan="1" <span style="font-size:100%; background:#ddeee1; text-align:left; border: 0px solid black; background:pale gray">|'''NOTES on abberancy'''
!colspan="2" style = "background:lightgrey; border:solid"| '''When to consder an amended lineage assignment'''</br>The criteria below are brief and only indicate where concern should be raised, please see link (in blue) for full information.
|-
|-
|colspan="1" style = "font-size:100%; background:#f7faf8"|'''Definition''' marker in AML when expressed (around 80% of cases). More frequent in cases with granulocytic maturation. When detected by flow cytometry is diagnostic of myeloid differentiation is established (either AML or MPAL)
!colspan="1" style = "background:#FFFFF0;border:solid"| Mixed Phenotype Acute Leukaemia</br>See: '''[[MPAL]]'''
!colspan="1" style = "background:white;border:solid; font-size:90%;"| Consider MPAL if: There is sufficient evidence to assign myeloid lineage '''but''' the cells also express either a lineage-defining marker of T or B cells, or more than one lineage associated marker of T or B cells.
|-
|-
|colspan="1" style = "font-size:100%;"|A '''lineage-defining''' marker in AML when expressed (around 80% of cases). More frequent in cases with granulocytic maturation. When detected by flow cytometry is diagnostic of myeloid differentiation is established (either AML or MPAL)
!colspan="1" style = "background:#FFFFF0;border:solid"| Acute Undifferentiated Leukaenmia</br>See: '''[[AUL]]'''
!colspan="1" style = "background:white; border:solid; font-size:90%;"| Consider AUL if: There is insufficient evidence to assign myeloid lineage, but there is expression of one myeloid-associated marker, '''and''' you cannot assign T-cell or B-cell lineage. I
|-
|-
|colspan="1" style = "font-size:100%;"|A '''lineage-defining''' marker in AML when expressed (around 80% of cases). More frequent in cases with granulocytic maturation. When detected by flow cytometry is diagnostic of myeloid differentiation is established (either AML or MPAL)
!colspan="1" style = "background:#FFFFF0;border:solid"| Non-haematological malignancy</br>See '''[[Non-aematological malignancy|Non-haem]]'''
|}
!colspan="1" style = "background:white; border:solid; font-size:90%;"| Consider non-haematological malignancy if: Myeloid markers are expressed but not conclusice, CD45 expression is very weak, the presentation is atypical.
</div>
 
B cell markers frequently expressed in AML: changes lineage assignment, may change assignment, does not change assignment
T cell markers frequently expressed in AML
 
MPAL
 
*Any '''myeloid lineage-defining''' marker is present but '''B-Lymphoid and/or T-lymphoid defining markers''' are also present
or
*'''At least two myeloid lineage-associated markers are present''' but also ''''two markers of B-lymphoid and/or T-lymphoid lineage''' are present
OR
*Cells have '''no more than one lineage-associated''' marker of any lineage
 
ETP-ALL
PCDCN
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‎<span id="anchor_3">‎</span>.
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{| class="wikitable" style="color:black; background-color:#ffffff;" cellpadding="0"
!colspan="2" <span style="font-size:90%; colour:white; text-align:center; border: 1px solid black; background:pale gray">|'''NON MYELOID MARKERS FREQUENTLY "ABERENTLY" EXPRESSED IN AML'''</span>
|-
|colspan="2" style = "font-size:90%; color:black; background:#eedddd" |Markers of lymphoid lineage indicating primitive dfferentiation in AML
<div class="mw-collapsible mw-collapsed" data-expandtext="Click for explanation" data-collapsetext="Hide explanation">
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<span style="font-size:90%;></br>Some additional markers are regarded as indicating primitive nature when expressed by AML blasts; these markers may be more usually assocated with T-lineage or B-lineage ALL, but when expressed in AML they are considered to indicate less differentiated forms.</br>
</span>
</div></div></div>
|-
|colspan="1" style = "width: 4%; font-size:90%; color:black; background:white" |'''[[TDT]]'''
|colspan="1" style = "font-size:80%; background:white;"|Expressed in some cases of AML (5-20%) particularly in less differentiated blast cells, often on a sub-population of cells. More typically associated with primitive ALL blast cells.
|-
|colspan="1" style = "font-size:90%; color:black; background:white" |'''[[CD7]]'''
|colspan="1" style = "font-size:80%;background:white "|Predominantly seen as a T-cell antigen, CD7 tends may be expressed by AML blasts (20-40%) where it most often indicates a more primitive forms or MPAL. CD7 is most consistently a marker of T-lineage (including T-ALL and more mature froms).
|-
|colspan="2" style = "font-size:90%; color:black; background:#eedddd" |Markers of lymphoid differentation abererantly expressed in AML
<div class="mw-collapsible mw-collapsed" data-expandtext="Click for explanation" data-collapsetext="Hide explanation">
<div class="mw-collapsible-content">
<span style="font-size:90%;></br>Some additional markers are regarded as indicating primitive nature when expressed by AML blasts; these markers may be more usually assocated with T-lineage or B-lineage ALL, but when expressed in AML they are considered to indicate less differentiated forms.</br>
</span>
</div></div></div>
|-
|colspan="1" style = "width: 4%; font-size:90%; color:black; background:white" |'''[[TDT]]'''
|colspan="1" style = "font-size:80%; background:white;"|Expressed in some cases of AML (5-20%) particularly in less differentiated blast cells, often on a sub-population of cells. More typically associated with primitive ALL blast cells.
|-
|colspan="1" style = "font-size:90%; color:black; background:white" |'''[[CD7]]'''
|colspan="1" style = "font-size:80%;background:white "|Predominantly seen as a T-cell antigen, CD7 tends may be expressed by AML blasts (20-40%) where it most often indicates a more primitive forms or MPAL. CD7 is most consistently a marker of T-lineage (including T-ALL and more mature froms).
|-
|}
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‎<span id="anchor_4">‎</span>.
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{| class="wikitable" style="color:black; background-color:#ffffff;" cellpadding="0"
 
!colspan="2" <span style="font-size:90%; text-align:center; border: 1px solid black; background:pale gray">|'''IMPORTANT ADDITIONAL POINTS 1'''</br></span>
|-
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1" |AML subtypes with distinctive phenotype
<div class="mw-collapsible mw-collapsed" data-expandtext="Click for explanation" data-collapsetext="Hide explanation">
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<span style="font-size:80%;></br>The first step in AML diagnosis to establish the primitive nature of the abnormal cells:</br>
 
<span style="font-size:80%;>'''(1)''' Typically AML blasts have low CD45 expression and cause low side scatter. This means that they form a relatively uniform and distinctive population that is clearly separate from that of lymphocytes on CD45/SSc plots ([[CD45|for further details see this section]]) also not all AML forms may fit this pattern - particularly [[APL]] and [[monocytic AML]].</br>
<span style="font-size:80%;>'''(2)''' Additional markers often expressed on myeloid cells may help confirm the primitive nature of the cells: in AML this is most often CD34, although other markers may contribute.</br>
</span>
</div></div></div>
|-
|colspan="2" style = "font-size:90%; color:black;" |'''Mixed Phenotype Acute leukaemia (MPAL)'''
|-
|colspan="2" style = "font-size:84%;"|Formerly known as leukaemia of ambiguous lineage
|-
|colspan="2" style = "font-size:90%; color:black;" |'''Early T-precursor acute lymphoblastic leukaemia (ETP-ALL)'''
|-
|colspan="2" style = "font-size:84%;"|A (relatively new entity)
|-
|-
!colspan="1" style = "background:#FFFFF0;border:solid"|Early T-cell precursor ALL</br>See: '''[[ETP-ALL]]'''
!colspan="1" style = "background:white; border:solid; font-size:90%;"| The marker pattern is of a primitive T cell neoplasm with lineage-defining crieria, but there are also myeloid markers expressed
|}
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<span id="anchor_5">‎</span>.
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{| class="wikitable" style="color:black; background-color:#ffffff;" cellpadding="0"
!colspan="2" <span style="font-size:90%; text-align:center; border: 1px solid black; background:pale gray">|'''IMPORTANT ADDITIONAL POINTS 2'''</br></span>
|-
|colspan="2" style = "font-size:90%; color:black; background:#ddeee1" |'''Acute leukaemias with ambiguous lineage features'''
<div class="mw-collapsible mw-collapsed" data-expandtext="Click for explanation" data-collapsetext="Hide explanation">
<div class="mw-collapsible-content">
<span style="font-size:80%;></br>The first step in AML diagnosis to establish the primitive nature of the abnormal cells:</br>
<span style="font-size:80%;>'''(1)''' Typically AML blasts have low CD45 expression and cause low side scatter. This means that they form a relatively uniform and distinctive population that is clearly separate from that of lymphocytes on CD45/SSc plots ([[CD45|for further details see this section]]) also not all AML forms may fit this pattern - particularly [[APL]] and [[monocytic AML]].</br>
<span style="font-size:80%;>'''(2)''' Additional markers often expressed on myeloid cells may help confirm the primitive nature of the cells: in AML this is most often CD34, although other markers may contribute.</br>
</span>
</div></div></div>
|-
|colspan="2" style = "font-size:90%; color:black;" |'''Mixed Phenotype Acute leukaemia (MPAL)'''
|-
|colspan="2" style = "font-size:84%;"|Formerly known as leukaemia of ambiguous lineage: Myeloid MPO or monocytic defined by at least two markers (CD14, CD11c, CD64, NSE, lysozyme. T lineage CD3 (s or m), STRONG Cd19, with strong CD79a cCD22 or CD10 OR wk CD19 also with obove
|-
|colspan="2" style = "font-size:90%; color:black;" |'''Early T-precursor acute lymphoblastic leukaemia (ETP-ALL)'''
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|colspan="2" style = "font-size:84%;"|A (relatively new entity)
|-
|colspan="2" style = "font-size:90%; color:black;" |'''Undifferentiated acute leukaeemia'''
|-
|colspan="2" style = "font-size:84%;"|A (relatively new entity)
|-
|colspan="2" style = "font-size:90%; color:black;" |'''Non-haematopoietic tumours'''
|-
|colspan="2" style = "font-size:84%;"|need to know problems
|-
|}
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Latest revision as of 16:52, 28 November 2023

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SECTION 1: Establishing the primitive nature of the blast cells in AML

AML M1.png

Blast cells are recognised by morphology using features such as primitive nuclear or basophilic cytoplasmic appearances; similar principles are applied in flow cytometry where particular markers suggest a more primitive nature.


Table: Markers primarily used to confirm primitive nature in AML.  
The expression of some markers is typically associated with primitive cells and can help recognise the primitive nature of blast cells.
Note that these markers may also have some lineage specificity but are not generally used to assign lineage
CD45 A marker expressed by all leukocytes and their precursors. In AML expression is characteristically "weak" i.e. significantly less intense than normal lymphocytes or monocytes. In monocytic AML expression may be stronger, particular in mare mature monocytic forms where expression may resemble normal monocytes.
CD34 Frequently expressed by AML blast cells (40-80% of cases) - most often in less differentiated forms of AML. Expression is also seen frequently (and often more strongly) in ALL
Other markers: In the context of a proven AML diagnosis a number of markers may be expressed that reflect the primitive nature of the cells. Some of these are more frequently associated with lymphoid disorders, but providing other criteria for AML are met they should simply be considered to show "primitivness".
These include: CD38, HLA-DR, TDT, CD7.


SECTION 2: Assigning blast cells as myeloid lineage i.e. Diagnosing AML

AML M2.png

In morphology other features are used to indicate myeloid lineage, some are highly specificsuch as Auer rods, others may suggest myeloid lineage but be less specific. Again similar principles apply in flow cytometry


There are two ways to make a diagnosis of AML

Requirements to diagnose AML by flow cytometry
Pattern 1:
A myeloid lineage-defining marker pattern is present
and
No lineage-defining markers of T or B cells are present 		See Table 1 for lineage-defining marker patterns in AML
Pattern 2:
At least two myeloid lineage-associated markers are present
and
There are no lineage defining markers of T or B cells
and
No more than one: T-cell or B-cell lineage-associated markers are present 		See Table 2A and Table 2B for lineage-associated markers in AML
Table 1
Myeloid-lineage defining markers in AML
Lineage is defined by either the definite assignment to myeloid lineage or definite assignment to monocytic lineage. In each case there are specific criteria.
Myeloperoxidase is expressed MPO is lineage-defining in AML (expressed in around 80% of cases)
Monocytic lineage can be assigned. This requires detection of at least two of: CD14, CD11c, CD64, NSE, lysozyme*
Table 2A
Myeloid lineage-associated markers (Main Set)
Each of these markers is supports a diagnosis of myeloid lineage, but are not AML-defining when expressed alone. However, in the absence of markers suggesting alternative lineage expression of two of these markers may be used to assign myeloid lineage.


CD117 An early marker of myeloid lineage, seen in up to 80% of AML and vauable in recognising more primitive differentaiion forms (note that aberrant expression is seen in up to 20% of ALL cases)
CD33 A good marker for AML, particularly for those cases with granulocytic maturation, CD33 is often less strongly expressed in AML with monocytic dfferentiation and strongly expressed in APL.
CD13 A good lineage marker for AML that is acquired a little later in differentation than CD117 or CD33; expression of CD13 is often higher than CD33 in AML with monocytic differentiation.
Table 2B
Myeloid lineage-associated markers (Specific differentiation)
The markers already described above are sufficient to make a diagnosis of typical AML in most cases. Typically the markers in this table are associated with specific features of differentiation so will not be present in all cases, but may be helpful as "lineage-assocated" markers in difficult cases. Care should be taken when doing so, since in some cases specificity may be lower than for typical myeloid markers.
Additional features of granulocytic maturation
CD11b A marker of both granulocytic and monocytic maturation, this marker has previously been associated with less good outcome in a number of studies
Addtional features of monocytic differentiation
CD11c This marker is most associated with monocytic maturation in AML being fairly well corellated with CD11B, but overall probably less specific for monocytic differentiation that CD14
CD14 Primarily a marker of monocytic maturation in AML, seen most often in more differentiated forms, when present CD14 be considered a strong indicator of monocytic phenotype.
CD64 A good lineage marker for monocytic differentiation in AML, expressed in both monoblastic and monocytic forms, not fully sepicific when expressed at lower levels.
Features associated with erythroid differentiation
Most often CD34, CD45 and HLA-DR are weak or negative, although CD117 and CD36 are generally expressed. There may be some expression of platelet markers in some cases.
CD71 Frequently expressed though not fully lineage specific
CD235 A good marker of erythroid differentiation but acquired late and therefore may not be expressed
Features associated with megakaryocytic differentiation
Most often CD34, CD45 and HLA-DR are weak or negative, although CD13 and CD33 may be expressed
CD41 Platelet glycoprotein IIbIIIa
CD61 Platelet glycoprotein IIIa
CD36 Relatively non-specific (seen in erythroid and monocytic leukaemias) but often strongly expressed



SECTION 3: When to consider alternative lineage assignment

The "aberrent" expression of lymphoid markers is frequently encountered in AML (and in some patterns of mutation these may be expected); however when non-myeloid markers are found it is important to consder if this changes lineage assignment. There are several conditions that should be considered:


When to consder an amended lineage assignment
The criteria below are brief and only indicate where concern should be raised, please see link (in blue) for full information.
Mixed Phenotype Acute Leukaemia
See: MPAL 		Consider MPAL if: There is sufficient evidence to assign myeloid lineage but the cells also express either a lineage-defining marker of T or B cells, or more than one lineage associated marker of T or B cells.
Acute Undifferentiated Leukaenmia
See: AUL 		Consider AUL if: There is insufficient evidence to assign myeloid lineage, but there is expression of one myeloid-associated marker, and you cannot assign T-cell or B-cell lineage. I
Non-haematological malignancy
See Non-haem 		Consider non-haematological malignancy if: Myeloid markers are expressed but not conclusice, CD45 expression is very weak, the presentation is atypical.
Early T-cell precursor ALL
See: ETP-ALL 		The marker pattern is of a primitive T cell neoplasm with lineage-defining crieria, but there are also myeloid markers expressed
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