HAEM5:T-large granular lymphocytic leukaemia: Difference between revisions

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 |WHO, NCCN
 |STAT3 mutation has been associated with statistically significant neutropenia, thrombocytopenia, and reduced numbers of most normal residual blood-leukocyte subsets<sup>[22]</sup>
 STAT3 mutations are associated with a worse prognosis and reduced overall survival <sup>[1][23]</sup>
 Patients with STAT 3 mutation required treatment more frequently when compared to patients with STAT3 wild type<sup>[18]</sup>
@@ Line 176: / Line 179: @@
-STAT3 mutation can also be seen in other T-cell lymphomas including hepatosplenic T-cell lymphoma<sup>[12]</sup>
+STAT3 mutation can also be seen in other T-cell lymphomas including hepatosplenic T-cell lymphoma<sup>[12]</sup>
+% of patients with STAT3 mutations, had multiple mutations in the STAT3 gene, solely in cytotoxic CD8+ or NK cells.<ref name=":4" />
 |-
 |STAT5B <sup>[1]</sup> <br />
@@ Line 196: / Line 202: @@
 Mutations in the inter-domain region: P702A <sup>[19]</sup>
 |Other <sup>[32]</sup>
-|Common <sup>[20]</sup>
+|Rare <sup>[7]</sup>
 |D,P,T
 |WHO, NCCN
 |N642H mutation (associated with more aggressive disease)<sup>[13][14]</sup>
 Clones can acquire multiple STAT5B mutations <sup>[19]</sup>
 STAT5B mutations can also be seen in other T-cell lymphomas including hepatosplenic T-cell lymphoma<sup>[12</sup>
 N642H mutation is associated with CD3+/CD56+ phenotype<sup>[14]</sup>
 STAT5B mutations are more common in CD4+ T-LGLL than in CD8+ T-LGLL <sup>[19][20]</sup>
@@ Line 233: / Line 241: @@
 |WHO
 |TNFAIP 3 mutation has been correlated with increased overall survival <sup>[17]</sup>
 TNFAIP3 itself is a NF‐κB target gene<sup>[15]</sup>
+In one study three of four of the patients with non‐synonymous TNFAIP3 alterations also harbored a STAT3 mutation (''p''  = 0.004)<sup>[9]</sup>
-In one study three of four of the patients with non‐synonymous TNFAIP3 alterations also harbored a STAT3 mutation (''p''  = 0.004)<sup>[9]</sup>
 |-
 |TET2 <sup>[1]</sup>
@@ Line 282: / Line 290: @@
 KMT2D has been how to exhibit significant co-occurrence with STAT3 mutation <sup>[26]</sup>
+|-
+|TRAF3 <sup>[30]</sup>
+|c.650A>T p.E217V <sup>[30]</sup>
+|Other <sup>[39]</sup>
+|Rare <sup>[30]</sup>
+|N/A
+|None
+|Mutated putative driver <sup>[30]</sup>
 |-
 |CLIP3 <sup>[30]</sup>
-|
+|c.908A>T p.D303V
-|
-|
-|
+c.917A>T p.K306M <sup>[30]</sup>
-|
+|Other <sup>[40]</sup>
-|
+|Rare <sup>[30]</sup>
+|N/A
+|None
+|Mutated putative driver <sup>[30]</sup>
+|-
+|FBXW2 <sup>[30]</sup>
+|c.683C>G p.A228G <sup>[30]</sup>
+|Other <sup>[41]</sup>
+|Rare <sup>[30]</sup>
+|N/A
+|None
+|Mutated putative driver <sup>[30]</sup>
+|-
+|CREBBP <sup>[30]</sup>
+|c.1178A>G p.N393S
+c.4306T>C p.C1436R <sup>[30]</sup>
+|Other
+|Rare <sup>[30]</sup>
+|N/A
+|None
+|A case is described of CCL22 co-occurring with a STAT3 mutation in a CD8+ TCR αβ T-LGLL<sup>[28]</sup>
+A case is described of CCL22 mutation co-occurring with both STAT3 and STAT5B in a CD4+TCR αβ T-LGLL <sup>[28]</sup>
 |}Note: A more extensive list of mutations can be found in [https://www.cbioportal.org/ <u>cBioportal</u>], [https://cancer.sanger.ac.uk/cosmic <u>COSMIC</u>], and/or other databases. When applicable, gene-specific pages within the CCGA site directly link to pertinent external content.
 <blockquote class="blockedit">{{Box-round|title=v4:Gene Mutations (SNV/INDEL)|The content below was from the old template. Please incorporate above.}}</blockquote>
-Somatic activating STAT3 and STAT5b mutations are the most common SNVs in T-LGL.
 {| class="wikitable sortable"
@@ Line 354: / Line 391: @@
 **An epigenetic inhibition mechanism to SOCS3 gene is hypothesized<ref name=":10" />
 **KIR3DL1 has been shown to be down-modulated by hypermethylation of the promoter<ref name=":10" />
+**Mutations in KMT2D and TET2 have been found to significantly co-occur with STAT3 mutations<sup>[26]</sup>
 <br />
@@ Line 365: / Line 403: @@
 !Gene; Genetic Alteration!!Pathway!!Pathophysiologic Outcome
 |-
-|<span class="blue-text">EXAMPLE:</span> ''BRAF'' and ''MAP2K1''; Activating mutations
+|JAK/STAT<sup>[7]</sup>
-|<span class="blue-text">EXAMPLE:</span> MAPK signaling
+|Constitutive activation
-|<span class="blue-text">EXAMPLE:</span> Increased cell growth and proliferation
+|Dysregulation of apoptosis
 |-
-|<span class="blue-text">EXAMPLE:</span> ''CDKN2A''; Inactivating mutations
+|NK-kB<sup>[7]</sup>
-|<span class="blue-text">EXAMPLE:</span> Cell cycle regulation
+|Pathway activation
-|<span class="blue-text">EXAMPLE:</span> Unregulated cell division
+|Preventing apoptosis
 |-
-|<span class="blue-text">EXAMPLE:</span> ''KMT2C'' and ''ARID1A''; Inactivating mutations
+|FAS and FASL<sup>[7]</sup>
-|<span class="blue-text">EXAMPLE:</span> Histone modification, chromatin remodeling
+|Resistance to FAS mediated apoptosis
-|<span class="blue-text">EXAMPLE:</span> Abnormal gene expression program
+|Activation of pro-survival pathways which is postulated to lead to neutropenia
 |-
-|
+|RAS/RAF1/MEK1/ERK<sup>[7]</sup>
-|
+|Overactive RAS
-|
+|Constitutive activation of RAS and ERK
+|-
+|PI3K/AKT<sup>[7]</sup>
+|Dysregulation
+|Apoptosis inhibition
 |}
 <blockquote class="blockedit">{{Box-round|title=v4:Genes and Main Pathways Involved|The content below was from the old template. Please incorporate above.}}</blockquote>
-*JAK/STAT<ref name=":9" />
+**
-**Constitutive activation
-*NK-κB<ref name=":9" />
-**Activation of this pathway
-**Preventing apoptosis
-*T-LGL's express high levels of FAS and FASL<ref name=":9">Lamy T, Moignet A, Loughran TP. LGL leukemia: from pathogenesis to treatment. Blood. 2017 Mar 2;129(9):1082-94.</ref>
-**Resistant to FAS mediated apoptosis
-**Leading to activation of prosurvival pathways
-**Postulated to lead to neutropenia seen in these patients.
-*RAS/RAF1/MEK1/ERK <ref name=":9" />
-**Overactive RAS
-**Constitutive activation of RAS and ERK
-*PI3K/AKT<ref name=":9" />
-**Dysregulation
-**Contributing to apoptosis inhibition
 <blockquote class="blockedit">
@@ Line 406: / Line 434: @@
 ==Genetic Diagnostic Testing Methods==
 *Morphologic assessment, flow cytometry and immunohistochemistry
 *PCR to assess for clonality, T-cell receptor (TCR) gene rearrangements
-**TCR gamma (TCRG) gene is rearranged in all cases, regardless of the type of TCR expressed, thus proves clonality<ref name=":0" />
+** TCR gamma (TCRG) gene is rearranged in all cases, regardless of the type of TCR expressed, thus proves clonality
-***Can be helpful in differentiating a reactive lymphocytosis from clonal T-LGL's
+** Can be helpful in differentiating a reactive lymphocytosis from clonal T-LGL's
-**NK LGL proliferations do not express TCR, making assessment of clonality difficult<ref name=":9" />
+*** NK LGL proliferations do not express TCR, making assessment of clonality difficult
-***Expression of activating isoforms of killer immunoglobulin-like receptors (KIR) can be used as a surrogate marker of clonality in NK LGL<ref name=":9" />
+*** Expression of activating isoforms of killer immunoglobulin-like receptors (KIR) can be used as a surrogate marker of clonality in NK LGL
+* Myeloid neoplasms may present with clonal large granular lymphocyte expansion with STAT3/STAT5B mutations. Next generation sequencing can be diagnostically useful in these cases<sup>[21]</sup>
 ==Familial Forms==
@@ Line 419: / Line 448: @@
 ==Additional Information==
-*N/A
+*PI3K-Akt has been found to be upregulated in KLRG1<sup>-</sup> CD8<sup>+</sup> T-LGLL. Studies are being conducted to examine treatment with linperlisib.<sup>[29]</sup>
+*Myleoid clonal hematopoiesis is associated with the presence of cytopenia in LGLL<sup>[30]</sup>
 ==Links==