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The flow cytometric diagnosis of AML: Difference between revisions

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[[Acute leukaemia types]]
 
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| colspan="1"''|[[Flow Cytometry|Return to previous page]]''
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*For most cases, the diagnosis of AML by flow cytometry is relatively straightforward, and can be addressed in a structured manner.
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*The key is to ensure atypical cases are identified and unusual diagnoses are not missed. The workflow here is based on WHO criteria.
{| class="wikitable" style="border-style: solid; border-width: 5px; color:black"
|colspan="1" style = "font-size:90%; color:black; background: #bcd4e6"|'''1. The immunophenotype of the blast cells should be consistent with their "primitive" nature'''
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[[Image:AML M1.png|110px]]
</br></br><span style="font-size:90%;">Assigning primitive nature in most cases is straightforward, but some types of AML may present difficulties.</span>


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{| class="wikitable" style="border-style: solid; border-width: 4px; color:black"
!colspan="1" style = "background:#ddeee1; border:solid; border-width: 3px;"|<span style="font-size:90%;">'''Demonstrating primitive phenotype in AML'''</span></br>
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!colspan="1" style = "background:white; border:solid; border-width: 1px; color:black"|In most cases, cells of AML will demonstrate typical features of immature cells with: '''weak expression of CD45''', and expression of '''CD34''' and/or '''CD117'''</br>However, patterns are not always typical and difficult cases other markers of early differentiation may also help</br></br>[[Markers used to demonstrate primitive nature in AML|''Click for a more detailed table of markers associated with primitive phenotype'']]
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!colspan="1" style = "background:#ddeee1;border:solid"|<span style="font-size:90%;">'''Difficulties may occur where blast cells have significant maturation so their primitive nature may be less easy to demonstrate.'''</span></br>
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!colspan="1" style = "background:white; border:solid; border-width: 1px;"|Difficulties are most frequently encountered in monocytic cases of AML, or in acute promyelocytic leukaemia (APL) (although occasionally in other types).</br></br>[[Atypical patterns of primitive marker expression in acute myeloid leukaemia|Click to see common patterns that may cause difficulty in assigning primitive phenotype]]
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'''Principle 1.''' '''The cells should show flow cytometric features consistent with a primitive nature'''</br>
[[Image:AML M1.png|130px]]  Blast cells typically have "primitive" morphology, the initial procedure is to ensure that the cells also express markers of early differentiation


*Most often in AML useful features of immature cells are ''weak expression of CD45'', and expression of ''CD34'' and/or ''CD117''. However, other markers may be useful (See [[Markers used to demonstrate primitive nature in AML]])
*Note that some cases there may be atypical features where primitive nature is less clear, this is most frequently encoutered in more mature monocytic cases of AML or in APL, but also in other circumstances (see table [[Atypical patterns of primitive marker expression in acute myeloid leukaemia]])
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Can we confirm myeloid nature?
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*Typical cases can generally be recognised by (see table for details)
{| class="wikitable" style="border-style: solid; border-width: 5px; color:black"
*Atypical cases can still be identified based on a minimal feature set (see table for details)
|colspan="1" style = "font-size:90%; color:black; background:#bcd4e6"|'''2. The immunophenotype of the blast cells should allow myeloid lineage to be assigned'''
*In unusual cases an extended marker panel may allow lineage assignment (see Table for details)
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[[Image:AML M2.png|130px]] 
 
 
<span style="font-size:90%;">The criteria to assign myeloid lineage in AML have been established, alternative sets of diagnostic criteria may be used (although many cases will meet more than one criteria set):
 
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{| class="wikitable" style="border-style: solid; border-width: 4px; color:black"
!colspan="1" style = "background:#ddeee1; border:solid; border-width: 3px;"|<span style="font-size:90%;">'''Pattern A: AML - diagnosis based on lineage-defining markers'''</span></br>
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!colspan="1" style = "background:white; border:solid; border-width: 1px; color:black"|A myeloid lineage-defining marker pattern is present '''and''' no lineage-defining markers of T or B cells are present</br></br>
<span style="font-size:100%;">[[Flow cytometry: Myeloid-defining markers|Click to view table of criteria]]</span>
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!colspan="1" style = "background:#ddeee1;border:solid"|<span style="font-size:90%;">'''Pattern B: AML - diagnosis based on myeloid-lineage-associated marker patterns'''</span></br>
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!colspan="1" style = "background:white; border:solid; border-width: 1px;"|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 marker is present</br></br>
<span style="font-size:90%;">[[Myeloid lineage-associated markers|Click to view table of criteria]]</span>
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!colspan="1" style = "background:#ddeee1;border:solid"|<span style="font-size:90%;">'''Pattern C: AML - diagnosis based on less frequent differentiation patterns'''</span></br>
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!colspan="1" style = "background:white; border:solid; border-width: 1px;"|In those rarer cases of erythroid or megakaryocytic differentiation, full myeloid criteria may not be met requiring these patterns to be specifically diagnosed.</br></br>
<span style="font-size:90%;">[[Marker patterns erythroid or megakaryocyte differentiation|Click to view table of criteria]]</span>
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Are there atypical features?
 
*Expected abberency
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*Feature that may give concern
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|colspan="1" style = "font-size:90%; color:black; background:#bcd4e6"|'''3. Alternative diagnoses in difficult cases'''
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[[Image:Lymphoblast.png|110px]]
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<span style="font-size:90%;"></br>In some cases myeloid markers may be present but full lineage may be unclear - in such cases it is important to consider possible alternative diagnoses</span></br>
 
 
<span style="font-size:90%;">Alternative potential diagnoses in difficult cases with myeloid marker expression:</span>
 
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{| class="wikitable" style="border-style: solid; border-width: 4px; color:black"
!colspan="2" style = "background:#ddeee1;border:solid"|<span style="font-size:90%;">'''Mixed Phenotype Acute Leukaemia''' (MPAL)</span>
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!colspan="2" style = "background:white;border:solid;"|Consider where myeloid lineage can be assigned based on '''lineage-specific''' patterns '''but''' the cells also have marker patterns that meet the criteria to assign T or B cell lineage.</br></br>[[Flow cytometry:MPAL|''Click for diagnostic criteria of MPAL'']]
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!colspan="2" style = "background:#ddeee1;border:solid;"|'''Acute Undifferentiated Leukaemia''' (AUL)
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!colspan="2" style = "background:white; border:solid;"|'''Consider AUL:''' In cases where the evidence is insufficient to assign myeloid lineage '''and''' there is insufficient evidence to assign to T-cell or B-cell lineage </br></br>[[Flow cytometry:AUL|''Click for diagnostic criteria of AUL'']]
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!colspan="2" style = "background:#ddeee1;border:solid"|'''Acute Leukaemia of ambiguous lineage not otherwise sepcified''' (ALAL-NOS)
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!colspan="2" style = "background:white; border:solid;"|'''Consider ALAL-NOS:''' if classification to specific lineage is not possible '''but''' blast cells cannot be classed as AUL or MPAL.</br></br>[[Flow cytometry:ALAL-NOS|''This is most often a useful provisional diagnosis - click here for details'']]</br>
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!colspan="2" style = "background:#ddeee1;border:solid"|''' Early T-cell precursor acute lymphoblastic leukaemia''' (ETP-ALL)
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!colspan="2" style = "background:white; border:solid;"| This disorder has diagnostic criteria sufficient to assign T cell lineage (cCD3 is expressed) but may express myeloid-associated antigens cases may share features with MPAL M/T</br></br>[[Flow cytometry:ETP-ALL|''Click for diagnostic criteria of ETP-ALL'']]
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!colspan="2" style = "background:#ddeee1;border:solid"|'''Blastic plasmacytoid dendritic cell neoplasm''' (BPDCN)
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!colspan="2" style = "background:white; border:solid;"|'''Consider BPDCN:''' Generally in cases that resemble AUL (rarely AML), most often with skin rash. A specific marker profile should be sought: expression of bright CD4 and/or CD56 is expected. CD33 is frequently expressed but other myeloid markers are less frequent and MPO and CD34 should be absent. Look for specific additional markers as described in the diagnostic criteria.</br></br>[[Flow cytometry:BPDCN|''Click for diagnostic criteria of BPDCN'']]
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</br></br><span style="font-size:90%;">'''FINAL NOTE''' Some "non-lineage" markers are frequently expressed in AML and may be associated with specific AML subtypes ([[Table of frequent aberrant markers in AML|Click here for further detail]]). Other features should give concern for alternative diagnosis (see the table below more detailed guidance).
 
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Latest revision as of 15:28, 15 March 2024

1. The immunophenotype of the blast cells should be consistent with their "primitive" nature

AML M1.png

Assigning primitive nature in most cases is straightforward, but some types of AML may present difficulties.

Demonstrating primitive phenotype in AML
In most cases, cells of AML will demonstrate typical features of immature cells with: weak expression of CD45, and expression of CD34 and/or CD117
However, patterns are not always typical and difficult cases other markers of early differentiation may also help

Click for a more detailed table of markers associated with primitive phenotype
Difficulties may occur where blast cells have significant maturation so their primitive nature may be less easy to demonstrate.
Difficulties are most frequently encountered in monocytic cases of AML, or in acute promyelocytic leukaemia (APL) (although occasionally in other types).

Click to see common patterns that may cause difficulty in assigning primitive phenotype


2. The immunophenotype of the blast cells should allow myeloid lineage to be assigned

AML M2.png


The criteria to assign myeloid lineage in AML have been established, alternative sets of diagnostic criteria may be used (although many cases will meet more than one criteria set):

Pattern A: AML - diagnosis based on lineage-defining markers
A myeloid lineage-defining marker pattern is present and no lineage-defining markers of T or B cells are present

Click to view table of criteria

Pattern B: AML - diagnosis based on myeloid-lineage-associated marker patterns
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 marker is present

Click to view table of criteria

Pattern C: AML - diagnosis based on less frequent differentiation patterns
In those rarer cases of erythroid or megakaryocytic differentiation, full myeloid criteria may not be met requiring these patterns to be specifically diagnosed.

Click to view table of criteria


3. Alternative diagnoses in difficult cases

Lymphoblast.png


In some cases myeloid markers may be present but full lineage may be unclear - in such cases it is important to consider possible alternative diagnoses


Alternative potential diagnoses in difficult cases with myeloid marker expression:

Mixed Phenotype Acute Leukaemia (MPAL)
Consider where myeloid lineage can be assigned based on lineage-specific patterns but the cells also have marker patterns that meet the criteria to assign T or B cell lineage.

Click for diagnostic criteria of MPAL
Acute Undifferentiated Leukaemia (AUL)
Consider AUL: In cases where the evidence is insufficient to assign myeloid lineage and there is insufficient evidence to assign to T-cell or B-cell lineage

Click for diagnostic criteria of AUL
Acute Leukaemia of ambiguous lineage not otherwise sepcified (ALAL-NOS)
Consider ALAL-NOS: if classification to specific lineage is not possible but blast cells cannot be classed as AUL or MPAL.

This is most often a useful provisional diagnosis - click here for details
Early T-cell precursor acute lymphoblastic leukaemia (ETP-ALL)
This disorder has diagnostic criteria sufficient to assign T cell lineage (cCD3 is expressed) but may express myeloid-associated antigens cases may share features with MPAL M/T

Click for diagnostic criteria of ETP-ALL
Blastic plasmacytoid dendritic cell neoplasm (BPDCN)
Consider BPDCN: Generally in cases that resemble AUL (rarely AML), most often with skin rash. A specific marker profile should be sought: expression of bright CD4 and/or CD56 is expected. CD33 is frequently expressed but other myeloid markers are less frequent and MPO and CD34 should be absent. Look for specific additional markers as described in the diagnostic criteria.

Click for diagnostic criteria of BPDCN



FINAL NOTE Some "non-lineage" markers are frequently expressed in AML and may be associated with specific AML subtypes (Click here for further detail). Other features should give concern for alternative diagnosis (see the table below more detailed guidance).

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