Extra: Difference between revisions

Latest revision as of 20:53, 13 June 2023

Summary

CD138 is a marker used to identify normal or malignant plasma cells with a high level of specificity, but does not discriminate normal from abnormal plasma cells and in some cases expression in myeloma may be low compared with normal plasma cells so sensitivity can be an issue. Abberancy of expression is low, but expression may be seen in lymphoplamacytic or marginal zone lymphomas (only on those cells that have plasma cell differentiation)

Normal expression and function

CD138 is a membrane protein that supports cell adhesion or binds cytokines and chemokines. In the hematopoietic system expression of CD138 is acquired by B lymphocytes as they develop into plasma cells.

Diagnostic role

Most often CD138 used in conjunction with CD38 to identify plasma cells in the diagnosis or monitoring of myeloma
There is very little aberrant expression, but neoplastic plasma cells may in some cases have weak, variable, or occasionally undetectable expression
Expression is also seen cells that have plasmacytic differentiation in lymphoplasmacytoid lymphoma or marginal zone lymphoma

Other useful information

Outside of haematopoiesis CD138 is expressed by squamous epithelium.

SUMMARY TABLES

Expression: primitive cell types Click (i) on table for additional information
AML	B ALL	Burkitt	T ALL	ETP ALL (i)	MPAL (i)	H.gones (i)
<5%	<5%	<5%	<5%	<5%	<5%	<5%

Expression: mature B cell neoplasms
CLL	MCL	FL	MZL	HCL	DLBCL	LPL	PCL
<5%	<5%	<5%	5-20%	<5%	5-20%	40-80%	80-100%

Notes: expression is usual in myeloma, and will occur on cells with plasma cell differentiation in LPL or MZL

Expression: mature T cell neoplasms
ATLL	CTCL Sezary	T-PLL	T-LGL	NK-LGL
limited	limited	limited	limited	limited

Notes: limited reports are consistent with expression being very uncommon in T-lymphoproliferative disorders

@@ Line 1: / Line 1: @@
-Lght chains form part of the B-cell receptor and may therefore be considered as a pan B-cell marker that is expressed from the late lymphoblast stage until plasma cell differentiation begins. Where cells express predomnantly kappa or lambda (light chain restriction) then clonality can be inferred.
+<div style="background-color: #E0EEEE; {{round corners}} padding: 2em 2em;  margin-right: 5px;">
-normal function and expression
-The immunoglobulin molecule (with either kappa or lambda light chain) forms the antigen-recognising portion of the B-cell receptor. Normal mature B cells therefore express light chains which are formed during pro-B to pre-B cell development appearing at the surface and remaining expressed on the cell surface until plasma cell development (when the immunoglobulin molecules become internal contaned within cytoplasmic secretory vesicles).
+:<span style="color:navy">'''Summary'''</span>
+:CD138 is a marker used to identify normal or malignant plasma cells with a high level of specificity, but does not discriminate normal from abnormal plasma cells and in some cases expression in myeloma may be low compared with normal plasma cells so sensitivity can be an issue. Abberancy of expression is low, but expression may be seen in lymphoplamacytic or marginal zone lymphomas (only on those cells that have plasma cell differentiation)
-what is its diagnostic role
-*Indication of stage: acquisition of surface light-chain expression does not occur until a late point in B-precursor cell development so is useful be used to indicate developmental stage in ALL. Similarly, surface expression is lost at the point of plasma cell differentiation so absence od surface expression can indicate plasma cell developmental stage.
+</div>
-*Indication of clonality: malignant b-cells arise from a single parent cell so express light chain of a single type (either kappa or lambda) - light chain restriction. In many cases some normal cells will also be present so light chains may be a mixture of kappa and lambda. However when there is a malignant clone, cells expressing either kappa or lambda will predominate. Studies most frequently suggest that if the kappa to lambda ratio is greater than 3 1 then the presence of a clonal population can be inferred (although correlation with other markers is needed).
-*Weak or absent light chain expression may be seen in DLBCL FL or CLL and more rarely in MCL or MZL: overall around 10% of B-lymphoproliferative disorders do not express surface light chain.
-summary tables
+<span style="color:navy">'''Normal expression and function'''</span>
-. expression by acute leukaemias and by
+CD138 is a membrane protein that supports cell adhesion or binds cytokines and chemokines. In the hematopoietic system expression of CD138 is acquired by B lymphocytes as they develop into plasma cells.
-rare pro-b all
-poss  early pre-b all
-poss  pre-b all
-hi  b all
-rare  pro-t all
-rare  mature-t all
-rare  aml
-poss  haemato-gones
-*  expressed by late haematogones
-. expression by b-lymphoproliferative disorders
-hi cll
-hi  pll**
-hi  mcl
+<span style="color:navy">'''Diagnostic role'''</span>
-hi  fl
-hi  hcl**
+*Most often CD138 used in conjunction with CD38 to identify plasma cells in the diagnosis or monitoring of myeloma
-hi  hclv  l
+*There is very little aberrant expression, but neoplastic plasma cells may in some cases have weak, variable, or occasionally undetectable expression
-hi  mzl
+*Expression is also seen cells that have plasmacytic differentiation in lymphoplasmacytoid lymphoma or marginal zone lymphoma
-hi  lpl
-poss  pcs
+<span style="color:navy">'''Other useful information'''</span>
+Outside of haematopoiesis CD138 is expressed by squamous epithelium.
+----
+<span style="color:navy">'''''SUMMARY TABLES'''''</span>
+{| class=wikitable style="text-align: center; font-size:80%; width: 87.5%; height 20px;"
+|-
+!colspan="7"|<span style="font-size:100%">'''Expression: primitive cell types'''  ''Click (i) on table for additional information'' </span></font>
+|-
+! AML !! B ALL !! Burkitt || T ALL !! ETP ALL ('''[[Early T Precursor ALL (ETP-ALL)|i]]''') !! MPAL ('''[[Mixed Phenotype Acute Leukaemia (MPAL)|i]]) || H.gones ('''[[Haematogones|i]]''')
+|-
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|-
+|}
+{| class=wikitable style="text-align: center; font-size:80%; width: 100%; height 20px;"
+|-
+!colspan="8"|'''Expression: mature B cell neoplasms'''
+|-
+! CLL !! MCL !!FL!! MZL !! HCL !! DLBCL || LPL !! PCL
+|-
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #66e0ff; color:black"|5-20%
+|style="width: 12.5%; background: #E6FAFF; color:black"|<5%
+|style="width: 12.5%; background: #66e0ff; color:black"|5-20%
+|style="width: 14.25%; background: #006699; color:white"|40-80%
+|style="width: 12.5%; background: #004466; color:white"|80-100%
+|-
+|}
+<span style="font-size:90%">'''Notes:''' expression is usual in myeloma, and will occur on cells with plasma cell differentiation in LPL or MZL</span>
+{| class=wikitable style="text-align: center; font-size:80%; width: 62.4%; height 40px;"
+|-
+!colspan="7"|'''Expression: mature T cell neoplasms'''
+|-
+! ATLL !! CTCL Sezary !! T-PLL !! T-LGL !! NK-LGL
+|-
+|style= "width: 20%; background: #FFE4E1; color:black"|limited
+|style="width: 20%; background: #FFE4E1; color:black"|limited
+|style="width: 20%; background: #FFE4E1; color:black"|limited
+|style= "width: 20%; background: #FFE4E1; color:black"|limited
+|style="width: 20%; background: #FFE4E1; color:black"|limited
+|-
+|}
+<span style="font-size:90%">'''Notes:''' limited reports are consistent with expression being very uncommon in T-lymphoproliferative disorders</span>
+----

Extra: Difference between revisions

From haematologyetc.co.uk

Latest revision as of 20:53, 13 June 2023