Integrated Genomic Analysis Implicates Haploinsufficiency of Multiple Chromosome 5q31.2 Genes in De Novo Myelodysplastic Syndromes Pathogenesis

Graubert, Timothy A.; Payton, Michelle A.; Shao, Jin; Walgren, Richard A.; Monahan, Ryan; Frater, John L.; Walshauser, Mark A.; Martin, Mike G.; Kasai, Yumi; Walter, Matthew J.

doi:10.1371/journal.pone.0004583

Cited by 50 publications

(45 citation statements)

References 23 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…25,26 In addition, other genes involved in cell cycle regulation, CDC25C and CDC23, and in chromatin modification, JMJD1B, a lysine-specific histone demethylase and previously described candidate ts gene from 5q 27 are localized in this segment. A recently described study of exon sequencing for all genes from this segment revealed no mutations in any of these genes, 28 further supporting the notion that the haploinsufficiency of one or more genes from this interval is the disease mechanism. It was described that the dual-specific phosphatase CDC25C is inhibited by lenalidomide and that expression of this gene was lower in AML and MDS with del(5q); 29 therefore, haplodeficiency of proteins might also have a role.…”

Section: Discussionsupporting

confidence: 70%

Comprehensive array CGH of normal karyotype myelodysplastic syndromes reveals hidden recurrent and individual genomic copy number alterations with prognostic relevance

et al. 2011

View full text Add to dashboard Cite

About 40% of patients with myelodysplastic syndromes (MDSs) present with a normal karyotype, and they are facing different courses of disease. To advance the biological understanding and to find molecular prognostic markers, we performed a highresolution oligonucleotide array study of 107 MDS patients (French American British) with a normal karyotype and clinical follow-up through the Duesseldorf MDS registry. Recurrent hidden deletions overlapping with known cytogenetic aberrations or sites of known tumor-associated genes were identified in 4q24 (TET2, 2x), 5q31.2 (2x), 7q22.1 (3x) and 21q22.12 (RUNX1, 2x). One patient with a 7q22.1 deletion had an additional 5q31.2 deletion of the acute myeloid leukemia/MDS region, the smallest deletion identified so far and including the putative tumor suppressor (ts) genes, EGR1 and CTNNA1. One TET2 deletion was homozygous and one heterozygous, with a missense mutation in the remaining allele, further supporting its role as a ts gene. Besides these recurrent alterations, additional individual imbalances were found in 34 cases; in total, 42/107 (39%) cases had genomic imbalances. These patients had an inferior survival as compared with the rest of the patients (P ¼ 0.002). This study emphasizes the heterogeneity of MDS, but points to interesting genes that may have diagnostic and prognostic impact.

show abstract

Section: Discussionsupporting

confidence: 70%

Comprehensive array CGH of normal karyotype myelodysplastic syndromes reveals hidden recurrent and individual genomic copy number alterations with prognostic relevance

et al. 2011

View full text Add to dashboard Cite

show abstract

“…Candidate generesequencing studies have not identified a biallelic gene mutation on either interval, suggesting that gene haploinsufficiency is the genetic mechanism contributing to MDS initiation and progression. 9 Using an shRNA screen in primary human CD34 ϩ cells, haploinsufficiency of RPS14 on the distal 5q33 region was found to contribute to the abnormal erythroid differentiation and apoptosis that is commonly observed in patients with the 5q Ϫ syndrome. 10 A mouse model that is haploinsufficient for Rps14 and 7 other genes is characterized by macrocytic anemia, further supporting the hypothesis that RPS14 haploinsufficiency is an important MDS-initiating event.…”

Section: Karyotype Abnormalities In Mds and Gene Haploinsufficiencymentioning

confidence: 99%

Genetics of Myelodysplastic Syndromes: New Insights

Graubert

Walter

2011

Hematology

Self Cite

View full text Add to dashboard Cite

Myelodysplastic syndromes (MDS) are a heterogenous group of hematologic malignancies characterized by clonal expansion of BM myeloid cells with impaired differentiation. The identification of recurrent mutations in MDS samples has led to new insights into the pathophysiology of these disorders. Of particular interest is the recent recognition that genes involved in the regulation of histone function (EZH2, ASXL1, and UTX) and DNA methylation (DNMT3A, IDH1/IDH2, and TET2) are recurrently mutated in MDS, providing an important link between genetic and epigenetic alterations in this disease. The mechanism by which these mutated genes contribute to disease pathogenesis is an active area of research, with a current focus on which downstream target genes may be affected. Recent advances from sequencing studies suggest that multiple mutations are required for MDS initiation and progression to acute myeloid leukemia (AML). The past several years have yielded many new insights, but the complete genetic landscape of MDS is not yet known. Moreover, few (if any) of the findings are sufficiently robust to be incorporated into routine clinical practice at this time. Additional studies will be required to understand the prognostic implications of these mutations for treatment response, progression to AML, and survival.

show abstract

“…[1][2][3] The commonly deleted segment in 5q31.2 has been mapped, 4,5 and mutational analysis of the residual nondeleted allele has not identified a classic tumorsuppressor gene. [4][5][6] Therefore, we and others hypothesize that haploinsufficiency of a gene(s) in 5q31.2, not the loss of both alleles, may be a critical initiating event in MDS pathogenesis and may contribute to acute myeloid leukemia (AML) transformation when combined with additional cooperating mutations.The minimally deleted region on chromosome 5q31.2 is distinct from the minimally deleted region on 5q33.1, 7 which is associated with the 5q minus syndrome and carries a lower risk of progressing to AML compared with 5q31.2 deletions. Haploinsufficiency of the RPS14 gene, located in the 5q33.1 region, causes abnormal erythroid differentiation and accelerated apoptosis both in vitro and in a murine knockout model, supporting its role in the pathogenesis of the 5q minus syndrome.…”

mentioning

confidence: 99%

“…HSPA9 mRNA levels are reduced by 50% in CD34 ϩ -purified hematopoietic progenitors isolated from patients with del(5q) MDS compared with MDS patients without del(5q) and normal control CD34 ϩ cells, consistent with haploinsufficient expression levels in del(5q) patients. 6 An N-ethyl-N-nitrosourea mutagenesis screen in zebrafish identified that a bi-allelic mutation in Hspa9 resulted in anemia, dysplastic immature erythroblasts, accelerated apoptosis, and leukopenia. 15 Heterozygous Hspa9 mutant fish also displayed accelerated apoptosis in erythroid cells consistent with ineffective hematopoiesis.…”

mentioning

confidence: 99%

Knockdown of Hspa9, a del(5q31.2) gene, results in a decrease in hematopoietic progenitors in mice

Chen¹,

Kambal²,

Krysiak³

et al. 2011

Blood

Self Cite

View full text Add to dashboard Cite

IntroductionThe myelodysplastic syndromes (MDS) are a group of clonal hematopoietic disorders exhibiting ineffective hematopoiesis characterized by peripheral blood cytopenias. Whole chromosome 5 loss or interstitial deletions spanning 1 copy of 5q31.2 are among the most common abnormalities detected by conventional cytogenetic analysis in de novo (6%-20% of patients) and therapyrelated MDS (up to 40% of patients). [1][2][3] The commonly deleted segment in 5q31.2 has been mapped, 4,5 and mutational analysis of the residual nondeleted allele has not identified a classic tumorsuppressor gene. [4][5][6] Therefore, we and others hypothesize that haploinsufficiency of a gene(s) in 5q31.2, not the loss of both alleles, may be a critical initiating event in MDS pathogenesis and may contribute to acute myeloid leukemia (AML) transformation when combined with additional cooperating mutations.The minimally deleted region on chromosome 5q31.2 is distinct from the minimally deleted region on 5q33.1, 7 which is associated with the 5q minus syndrome and carries a lower risk of progressing to AML compared with 5q31.2 deletions. Haploinsufficiency of the RPS14 gene, located in the 5q33.1 region, causes abnormal erythroid differentiation and accelerated apoptosis both in vitro and in a murine knockout model, supporting its role in the pathogenesis of the 5q minus syndrome. 8,9 Deletions on the long arm of chromosome 5 typically encompass both 5q31.2 and 5q33.1 minimally deleted regions, suggesting that haploinsufficiency of multiple genes may be necessary to recapitulate the full spectrum of abnormalities observed in patients with MDS. Haploinsufficiency of Egr1 (located on 5q31.2), Apc (located proximal to the 5q31.2 minimally deleted region), or Npm (located distal to the 5q31.2 minimally deleted region) are associated with abnormal hematopoiesis in mice, further supporting the possibility that the deletion of multiple 5q genes may cooperate in MDS initiation or progression. [10][11][12][13][14] We hypothesized that haploinsufficiency of HSPA9, a gene located on the 5q31.2 interval, may also influence hematopoiesis in MDS patients based on several observations. HSPA9 mRNA levels are reduced by 50% in CD34 ϩ -purified hematopoietic progenitors isolated from patients with del(5q) MDS compared with MDS patients without del(5q) and normal control CD34 ϩ cells, consistent with haploinsufficient expression levels in del(5q) patients. 6 An N-ethyl-N-nitrosourea mutagenesis screen in zebrafish identified that a bi-allelic mutation in Hspa9 resulted in anemia, dysplastic immature erythroblasts, accelerated apoptosis, and leukopenia. 15 Heterozygous Hspa9 mutant fish also displayed accelerated apoptosis in erythroid cells consistent with ineffective hematopoiesis. 15 In mice, Hspa9 is a gene in the 5q31.2 interval that is a common retroviral insertional mutagenesis site associated with development of AML (see the Mouse Retrovirus Tagged Cancer Gene Database at: http://rtcgd.ncifcrf.gov/). 16 Finally, HSPA9 was identified as a mediator o...

show abstract

Integrated Genomic Analysis Implicates Haploinsufficiency of Multiple Chromosome 5q31.2 Genes in De Novo Myelodysplastic Syndromes Pathogenesis

Cited by 50 publications

References 23 publications

Comprehensive array CGH of normal karyotype myelodysplastic syndromes reveals hidden recurrent and individual genomic copy number alterations with prognostic relevance

Comprehensive array CGH of normal karyotype myelodysplastic syndromes reveals hidden recurrent and individual genomic copy number alterations with prognostic relevance

Genetics of Myelodysplastic Syndromes: New Insights

Knockdown of Hspa9, a del(5q31.2) gene, results in a decrease in hematopoietic progenitors in mice

Contact Info

Product

Resources

About