Jens Tiesmeier scite author profile

Mutations in RBM20 encoding the RNA-binding motif protein 20 (RBM20) are associated with an early onset and clinically severe forms of cardiomyopathies. Transcriptome analyses revealed RBM20 as an important regulator of cardiac alternative splicing. RBM20 mutations are especially localized in exons 9 and 11 including the highly conserved arginine and serine-rich domain (RS domain). Here, we investigated in several cardiomyopathy patients, the previously described RBM20-mutation p.Pro638Leu localized within the RS domain. In addition, we identified in a patient the novel mutation p.Val914Ala localized in the (glutamaterich) Glu-rich domain of RBM20 encoded by exon 11. Its impact on the disease was investigated with a novel TTN-and RYR2-splicing assay based on the patients' cardiac messenger RNA. Furthermore, we showed in cell culture and in human cardiac tissue that mutant RBM20-p.Pro638Leu is not localized in the nuclei but causes an abnormal cytoplasmic localization of the protein. In contrast the splicing deficient RBM20-p.Val914Ala has no influence on the intracellular localization. These results indicate that disease-associated variants in RBM20 lead to aberrant splicing through different pathomechanisms dependent on the localization of the mutation. This might have an impact on the future development of therapeutic strategies for the treatment of RBM20-induced cardiomyopathies.

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The emergence of a C/EBPα mutation in the clonal evolution of MDS towards secondary AML

Kaeferstein

Krug

Tiesmeier

et al. 2003

Leukemia

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Recently, mutations in the transcription factor CCAAT/ enhancer binding protein alpha (C/EBP␣) have been described in acute myeloid leukemia (AML). We performed a mutational analysis of the C/EBP␣ gene in the myelodysplastic syndromes and AML with antecedent MDS. No mutations were found in patients with refractory anemia (0/27), refractory anemia with ringed sideroblasts (0/7), refractory anemia with excess of blasts (RAEB 0/16) or chronic myelomonocytic leukemia (CMML 0/5). One out of 13 patients with RAEB-T/AML secondary to MDS showed a mutation in the C/EBP␣ gene. In this patient a 4 bp insertion disrupted codon 69 in one allele. This novel +1 frame shift is predicted to result in a truncated protein of 107 amino acids. However, the dominant protein translated was the C/EBP␣ isoform p30, which was previously shown to inhibit the DNA-binding and transactivation properties of C/EBP␣ p42. Interestingly this mutation could not be detected at diagnosis in the initial RAEB and RAEB-T stage. The mutation appeared at relapse after chemotherapy for RAEB-T. We conclude that the C/EBP␣ mutation was not essential for the initial blast accumulation. The emergence of a bast clone carrying a C/EBP␣ mutation at relapse indicates that this mutation may confer a growth advantage in a myeloid cell with an established differentiation block.

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Evolution of FLT3-ITD and D835 activating point mutations in relapsing acute myeloid leukemia and response to salvage therapy

et al. 2004

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Jens Tiesmeier

Cardiomyopathy‐associated mutations in the RS domain affect nuclear localization of RBM20

The emergence of a C/EBPα mutation in the clonal evolution of MDS towards secondary AML

Evolution of FLT3-ITD and D835 activating point mutations in relapsing acute myeloid leukemia and response to salvage therapy

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