Publication: Correlation of plasma cell assessment by phenotypic methods and molecular profiles by NGS in patients with plasma cell dyscrasias.
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| cris.virtualsource.author-orcid | 844b53d6-bf2e-4c0a-80f2-16ae33200688 | |
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| cris.virtualsource.author-orcid | 3ffc609d-4653-413a-a80f-2bf6c2b71f47 | |
| datacite.rights | open.access | |
| dc.contributor.author | Rebmann-Chigrinova, Ekaterina | |
| dc.contributor.author | Porret, Naomi | |
| dc.contributor.author | Andres, Martin | |
| dc.contributor.author | Wiedemann, Gertrud | |
| dc.contributor.author | Banz Wälti, Yara Sarah | |
| dc.contributor.author | Legros, Myriam | |
| dc.contributor.author | Pollak, Matthias | |
| dc.contributor.author | Oppliger Leibundgut, Elisabeth | |
| dc.contributor.author | Pabst, Thomas Niklaus | |
| dc.contributor.author | Bacher, Vera Ulrike | |
| dc.date.accessioned | 2024-10-11T17:17:19Z | |
| dc.date.available | 2024-10-11T17:17:19Z | |
| dc.date.issued | 2022-09-23 | |
| dc.description.abstract | BACKGROUND Next-generation sequencing (NGS) detects somatic mutations in a high proportion of plasma cell dyscrasias (PCD), but is currently not integrated into diagnostic routine. We correlated NGS data with degree of bone marrow (BM) involvement by cytomorphology (BMC), histopathology (BMH), and multiparameter flow cytometry (MFC) in 90 PCD patients. METHODS Of the 90 patients the diagnoses comprised multiple myeloma (n = 77), MGUS (n = 7), AL-amyloidosis (n = 4) or solitary plasmocytoma (n = 2). The NGS panel included eight genes CCND1, DIS3, EGR1, FAM46C (TENT5C), FGFR3, PRDM1, TP53, TRAF3, and seven hotspots in BRAF, IDH1, IDH2, IRF4, KRAS, NRAS. RESULTS Mutations were detected in 64/90 (71%) of cases. KRAS (29%), NRAS (16%) and DIS3 (16%) were most frequently mutated. At least one mutation/sample corresponded to a higher degree of BM involvement with a mean of 11% pathologic PC by MFC (range, 0.002-62%), and ~ 50% (3-100%) as defined by both BMC and BMH. CONCLUSIONS The probability of detecting a mutation by NGS in the BM was highest in samples with > 10% clonal PC by MFC, or > 20% PC by BMC/ BMH. We propose further evaluation of these thresholds as a practical cut-off for processing of samples by NGS at initial PCD diagnosis. | |
| dc.description.sponsorship | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| dc.description.sponsorship | Institut für Pathologie | |
| dc.description.sponsorship | Universitätsklinik für Medizinische Onkologie | |
| dc.identifier.doi | 10.48350/173251 | |
| dc.identifier.pmid | 36138464 | |
| dc.identifier.publisherDOI | 10.1186/s12920-022-01346-1 | |
| dc.identifier.uri | https://boris-portal.unibe.ch/handle/20.500.12422/87711 | |
| dc.language.iso | en | |
| dc.publisher | BioMed Central | |
| dc.relation.ispartof | BMC medical genomics | |
| dc.relation.issn | 1755-8794 | |
| dc.relation.organization | DCD5A442C055E17DE0405C82790C4DE2 | |
| dc.relation.organization | DCD5A442C448E17DE0405C82790C4DE2 | |
| dc.relation.organization | DCD5A442BF89E17DE0405C82790C4DE2 | |
| dc.subject | Bone marrow aspirate Flow cytometry Histopathology Multiple myeloma NGS Trephine biopsy | |
| dc.subject.ddc | 600 - Technology::610 - Medicine & health | |
| dc.subject.ddc | 500 - Science::570 - Life sciences; biology | |
| dc.title | Correlation of plasma cell assessment by phenotypic methods and molecular profiles by NGS in patients with plasma cell dyscrasias. | |
| dc.type | article | |
| dspace.entity.type | Publication | |
| dspace.file.type | text | |
| oaire.citation.issue | 1 | |
| oaire.citation.startPage | 203 | |
| oaire.citation.volume | 15 | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Institut für Pathologie | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| oairecerif.author.affiliation | Universitätsklinik für Medizinische Onkologie | |
| oairecerif.author.affiliation | Universitätsklinik für Hämatologie und Hämatologisches Zentrallabor | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.contributor.role | creator | |
| unibe.date.licenseChanged | 2022-09-26 09:41:56 | |
| unibe.description.ispublished | pub | |
| unibe.eprints.legacyId | 173251 | |
| unibe.refereed | true | |
| unibe.subtype.article | journal |
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