HAEM5:B-lymphoblastic leukaemia/lymphoma with hypodiploidy: Difference between revisions

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 ==Individual Region Genomic Gain/Loss/LOH==
-Please refer to section "Characteristic Chromosomal or Other Global Mutational Patterns" below.
+Hypodiploid B-ALL is characterized by widespread genomic losses consistent with the hypodiploid karyotype<ref name=":13" />. Please refer to section "Characteristic Chromosomal or Other Global Mutational Patterns" below.
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 </blockquote>
 ==Characteristic Chromosomal or Other Global Mutational Patterns==
-This entity is defined by the presence of neoplastic lymphoblasts containing less than 46 chromosomes<ref name=":0">Borowitz MJ, et al., (2017). B-Lymphoblastic leukaemia/lymphoma with recurrent genetic abnormalities, in World Health Organization Classification of Tumours of Haematopoietic and Lymphoid Tissues, Revised 4th edition. Swerdlow SH, Campo E, Harris NL, Jaffe ES, Pileri SA, Stein H, Thiele J, Arber DA, Hasserjian RP, Le Beau MM, Orazi A, and Siebert R, Editors. IARC Press: Lyon, France, p206.</ref>, and can be subdivided into near-haploid B-ALL/LBL with hypodiploidy (24–31 chromosomes); low-hypodiploid B-ALL/LBL with hypodiploidy (32–39 chromosomes); and high-hypodiploid B-ALL/LBL with hypodiploidy (40–43 chromosomes)<ref name=":13" /><ref name=":18">{{Cite journal|last=Harrison|first=Christine J.|last2=Moorman|first2=Anthony V.|last3=Broadfield|first3=Zoë J.|last4=Cheung|first4=Kan L.|last5=Harris|first5=Rachel L.|last6=Reza Jalali|first6=G.|last7=Robinson|first7=Hazel M.|last8=Barber|first8=Kerry E.|last9=Richards|first9=Sue M.|date=2004|title=Three distinct subgroups of hypodiploidy in acute lymphoblastic leukaemia|url=https://www.ncbi.nlm.nih.gov/pubmed/15147369|journal=British Journal of Haematology|volume=125|issue=5|pages=552–559|doi=10.1111/j.1365-2141.2004.04948.x|issn=0007-1048|pmid=15147369}}</ref>. Of note, near-diploid cases (44–45 chromosomes) are not included in the hypodiploid category in clinical therapy–directed classification schemes because they do not share the poor prognosis observed<ref name=":14" />. In a study, for patients with 44 chromosomes, monosomy 7, the presence of a dicentric chromosome, or both predicted a worse event-free survival (EFS) but similar overall survival (OS)<ref name=":3">{{Cite journal|last=Nachman|first=James B.|last2=Heerema|first2=Nyla A.|last3=Sather|first3=Harland|last4=Camitta|first4=Bruce|last5=Forestier|first5=Erik|last6=Harrison|first6=Christine J.|last7=Dastugue|first7=Nicole|last8=Schrappe|first8=Martin|last9=Pui|first9=Ching-Hon|date=2007|title=Outcome of treatment in children with hypodiploid acute lymphoblastic leukemia|url=https://www.ncbi.nlm.nih.gov/pubmed/17473063|journal=Blood|volume=110|issue=4|pages=1112–1115|doi=10.1182/blood-2006-07-038299|issn=0006-4971|pmc=1939895|pmid=17473063}}</ref>.
+This entity is defined by the presence of neoplastic lymphoblasts containing less than 46 chromosomes, and can be subdivided into near-haploid B-ALL/LBL with hypodiploidy (24–31 chromosomes); low-hypodiploid B-ALL/LBL with hypodiploidy (32–39 chromosomes); and high-hypodiploid B-ALL/LBL with hypodiploidy (40–43 chromosomes)<ref name=":13" /><ref name=":18">{{Cite journal|last=Harrison|first=Christine J.|last2=Moorman|first2=Anthony V.|last3=Broadfield|first3=Zoë J.|last4=Cheung|first4=Kan L.|last5=Harris|first5=Rachel L.|last6=Reza Jalali|first6=G.|last7=Robinson|first7=Hazel M.|last8=Barber|first8=Kerry E.|last9=Richards|first9=Sue M.|date=2004|title=Three distinct subgroups of hypodiploidy in acute lymphoblastic leukaemia|url=https://www.ncbi.nlm.nih.gov/pubmed/15147369|journal=British Journal of Haematology|volume=125|issue=5|pages=552–559|doi=10.1111/j.1365-2141.2004.04948.x|issn=0007-1048|pmid=15147369}}</ref>. Of note, near-diploid cases (44–45 chromosomes) are not included in the hypodiploid category in clinical therapy–directed classification schemes because they do not share the poor prognosis observed<ref name=":14" />. In a study, for patients with 44 chromosomes, monosomy 7, the presence of a dicentric chromosome, or both predicted a worse event-free survival (EFS) but similar overall survival (OS)<ref name=":3">{{Cite journal|last=Nachman|first=James B.|last2=Heerema|first2=Nyla A.|last3=Sather|first3=Harland|last4=Camitta|first4=Bruce|last5=Forestier|first5=Erik|last6=Harrison|first6=Christine J.|last7=Dastugue|first7=Nicole|last8=Schrappe|first8=Martin|last9=Pui|first9=Ching-Hon|date=2007|title=Outcome of treatment in children with hypodiploid acute lymphoblastic leukemia|url=https://www.ncbi.nlm.nih.gov/pubmed/17473063|journal=Blood|volume=110|issue=4|pages=1112–1115|doi=10.1182/blood-2006-07-038299|issn=0006-4971|pmc=1939895|pmid=17473063}}</ref>.
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 |No (NCCN)
 |Chromosome abnormalities include whole chromosome loss, specifically one sex chromosome and often chromosomes 7, 9, and/or 13.  Also detected are structural anomalies especially dicentric chromosomes involving chromosomes 7, 9 or 12.
-|}
+|}<blockquote class="blockedit">
+<center>
-<blockquote class="blockedit"></blockquote><blockquote class="blockedit">
-<center><span style="color:Maroon">'''End of V4 Section'''</span>
 ----
 </blockquote>
 ==Gene Mutations (SNV/INDEL)==
+Holmfeldt et al sequenced 124 cases of low-hypodiploid B-ALL and showed that more than two-thirds (70.6%) of near-haploid ALL cases harbored genetic alterations known or predicted to result in activation of RTK or Ras signaling, including deletion, amplification and/or sequence mutation of ''NF1'', ''NRAS'', ''KRAS'', ''MAPK1'', ''FLT3'' or ''PTPN11<ref name=":2" />''.
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@@ Line 165: / Line 163: @@
 |-
 |''NF1''
-|Mutations and focal deletions. In 68% of the cases, the ''NF1'' deletions were intragenic involving exons 15 through 35<ref name=":2" />.
+|Mutations and focal deletions. In 68% of the cases, the ''NF1'' deletions were intragenic involving exons 15 through 35. Because of aneuploidy, the ''NF1'' alterations were biallelic in 76.7% of near-haploid cases.<ref name=":2" />
 |Tumor supressor gene
 |Mutations: Recurrent
@@ Line 174: / Line 172: @@
 |-
 |''FLT3''
-|Mutations<ref name=":2" />
+|Mutation<ref name=":2" />
 |Oncogene
 |Recurrent
@@ Line 181: / Line 179: @@
 |-
 |''NRAS''
-|Mutations<ref name=":2" />
+|Mutation<ref name=":2" />
 |Oncogene
 |Recurrent
@@ Line 217: / Line 215: @@
 |-
 |''IKZF2''
-|Focal deletion<ref name=":16" />
+|Focal deletion. Alterations of ''IKZF2'' and ''IKZF3'' were biallelic as a result of aneuploidy<ref name=":2" />.
 |Tumor supressor
 |Common
@@ Line 226: / Line 224: @@
 |''IKZF3''
 <br />
-|Focal deletion<ref name=":16" />
+|Focal deletion and one frameshift mutation<ref name=":2" />
 |Tumor supressor
 |Recurrent
@@ Line 234: / Line 232: @@
 |-
 |''PAG1''
-|Focal deletion<ref name=":2" />
+|Focal deletion<ref name=":2" />. Most ''PAG1'' deletions were homozygous and involved the upstream region and first exon, leading to a complete loss of ''PAG1'' expression.
 |Tumor supressor
 |Recurrent
@@ Line 247: / Line 245: @@
 ==Epigenomic Alterations==
-In near haploid 19% of the cases had focal deletions of histone gene cluster at 6p22, however, non-hypodiploid ALL had 8%, lower frequency of these deletions<ref name=":2" />.
+In near haploid 19% of the cases had focal deletions of histone gene cluster at 6p22, however, non-hypodiploid ALL had 8%, lower frequency of these deletions<ref name=":2" />.  Of the 25 next generation sequenced haploid cases 16 (64%) cases had twenty six histone modifier gene mutations and of the 15 low hypodiploid ALL cases 9 (60%) cases had 9 mutations; the most common mutation (32%) of the near haploid cases was transcriptional co-activator and histone acetyltransferase ''CREBBP''<ref name=":2" />.
-Of the 25 next generation sequenced haploid cases 16 (64%) cases had twenty six histone modifier gene mutations and of the 15 low hypodiploid ALL cases 9 (60%) cases had 9 mutations; the most common mutation (32%) of the near haploid cases was transcriptional co-activator and histone acetyltransferase ''CREBBP''<ref name=":2" />.
 ==Genes and Main Pathways Involved==
@@ Line 260: / Line 256: @@
 |Constitutive activation of mitogenic and anti-apoptotic pathways, driving uncontrolled cell proliferation, survival, and malignant transformation.
 |-
-|''IKZF1, IKZF2, IKZF3, PAX5, EBF1, VPREB1''
+|''CDKN2A/B, TP53, RB1''; Loss of function mutations<ref name=":2" />
-|B-cell development
-|
-|-
-|''CDKN2A/B, TP53, RB1''; Loss of function mutations
 |Cell cycle and apoptosis
 |Propagation of genetically altered cells.
 |-
-|''ETV6''
+|''IKZF1, IKZF2, IKZF3, PAX5, EBF1, VPREB1''<ref name=":16" />
-|Hematopoiesis
+|B-cell development
-|
+|Altered lymphoid development and differentiation.
 |-
-|''PAG1''
+|''PAG1<ref name=":16" />''
 |BCR signaling
-|
+|Altered regulatory function in proximal B cell–receptor signaling.
+|-
+|''ETV6<ref name=":16" />''
+|Hematopoiesis
+|Not fully elucidated in this entity
 |-
-|''ARPP21''
+|''ARPP21<ref name=":16" />''
 |Calmodulin signaling
-|
+|Not fully elucidated in this entity
 |-
-|''SLX4IP''
+|''SLX4IP<ref name=":16" />''
 |Telomere length maintenance
-|
+|Not fully elucidated in this entity
 |-
-|''CUL5''
+|''CUL5<ref name=":16" />''
 |Ubiquitin pathway
-|
+|Not fully elucidated in this entity
 |-
-|''FAM53B''
+|''FAM53B<ref name=":16" />''
 |Wnt signaling
-|
+|Not fully elucidated in this entity
 |-
-|''PDS5B''
+|''PDS5B<ref name=":16" />''
 |Cohesis complex
-|
+|Not fully elucidated in this entity
 |-
-|''ANKRD11, DMD''
+|''ANKRD11, DMD<ref name=":16" />''
 |Cell adhesion
-|
+|Not fully elucidated in this entity
 |}
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+<blockquote class="blockedit"><center>
-<center>
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