• Something wrong with this record ?

SMARCB1-deficient sinonasal adenocarcinoma: a rare variant of SWI/SNF-deficient malignancy often misclassified as high-grade non-intestinal-type sinonasal adenocarcinoma or myoepithelial carcinoma

A. Skálová, T. Taheri, M. Bradová, T. Vaněček, A. Franchi, D. Slouka, T. Kostlivý, G. de Rezende, J. Michálek, N. Klubíčková, N. Ptáková, A. Nemcová, M. Michal, A. Agaimy, I. Leivo

. 2024 ; 485 (2) : 245-256. [pub] 20231212

Language English Country Germany

Document type Journal Article

Persistent link   https://www.medvik.cz/link/bmc24019626
E-resources Online Full text

NLK ProQuest Central from 2003-01-01 to 1 year ago
Medline Complete (EBSCOhost) from 2011-01-01 to 1 year ago
Nursing & Allied Health Database (ProQuest) from 2003-01-01 to 1 year ago
Health & Medicine (ProQuest) from 2003-01-01 to 1 year ago

Links

PubMed 38085333
DOI 10.1007/s00428-023-03650-2
Knihovny.cz E-resources

SMARCB1-deficient sinonasal adenocarcinoma is a rare variant of SWI/SNF-deficient malignancies with SMARCB1 loss and adenocarcinoma features. More than 200 high-grade epithelial sinonasal malignancies were retrieved. A total of 14 cases exhibited complete SMARCB1 (INI1) loss and glandular differentiation. SMARCA2 and SMARCA4 were normal, except for one case with a loss of SMARCA2. Next-generation sequencing (NGS) and/or fluorescence in situ hybridization (FISH) revealed an alteration in the SMARCB1 gene in 9/13 cases, while 2/13 were negative. Two tumors harbored SMARCB1 mutations in c.157C > T p.(Arg53Ter) and c.842G > A p.(Trp281Ter). One harbored ARID1B mutations in c.1469G > A p.(Trp490Ter) and MGA c.3724C > T p.(Arg1242Ter). Seven tumors had a SMARCB1 deletion. One carried an ESR1 mutation in c.644-2A > T, and another carried a POLE mutation in c.352_374del p.(Ser118GlyfsTer78). One case had a PAX3 mutation in c.44del p.(Gly15AlafsTer95). Histomorphology of SMARCB1-deficient adenocarcinoma was oncocytoid/rhabdoid and glandular, solid, or trabecular in 9/14 cases. Two had basaloid/blue cytoplasm and one showed focal signet ring cells. Yolk sac tumor-like differentiation with Schiller-Duval-like bodies was seen in 6/14 cases, with 2 cases showing exclusively reticular-microcystic yolk sac pattern. Follow-up of a maximum of 26 months (median 10 months) was available for 8/14 patients. Distant metastasis to the lung, liver, mediastinum, bone, and/or retroperitoneum was seen in 4/8 cases. Locoregional failure was seen in 75% of patients, with 6/8 local recurrences and 3 cervical lymph node metastases. At the last follow-up, 5 of 8 (62%) patients had died of their disease 2 to 20 months after diagnosis (median 8.2 months), and 3 were alive with the disease. The original diagnosis was usually high-grade non-intestinal-type adenocarcinoma or high-grade myoepithelial carcinoma. A correct diagnosis of these aggressive tumors could lead to improved targeted therapies with potentially better overall disease-specific survival.

References provided by Crossref.org

000      
00000naa a2200000 a 4500
001      
bmc24019626
003      
CZ-PrNML
005      
20241024110617.0
007      
ta
008      
241015s2024 gw f 000 0|eng||
009      
AR
024    7_
$a 10.1007/s00428-023-03650-2 $2 doi
035    __
$a (PubMed)38085333
040    __
$a ABA008 $b cze $d ABA008 $e AACR2
041    0_
$a eng
044    __
$a gw
100    1_
$a Skálová, Alena $u Department of Pathology, Faculty of Medicine in Pilsen, Charles University, E. Benese 13, 305 99, Pilsen, Czech Republic. skalova@biopticka.cz $u Bioptic Laboratory, Ltd., Pilsen, Czech Republic. skalova@biopticka.cz
245    10
$a SMARCB1-deficient sinonasal adenocarcinoma: a rare variant of SWI/SNF-deficient malignancy often misclassified as high-grade non-intestinal-type sinonasal adenocarcinoma or myoepithelial carcinoma / $c A. Skálová, T. Taheri, M. Bradová, T. Vaněček, A. Franchi, D. Slouka, T. Kostlivý, G. de Rezende, J. Michálek, N. Klubíčková, N. Ptáková, A. Nemcová, M. Michal, A. Agaimy, I. Leivo
520    9_
$a SMARCB1-deficient sinonasal adenocarcinoma is a rare variant of SWI/SNF-deficient malignancies with SMARCB1 loss and adenocarcinoma features. More than 200 high-grade epithelial sinonasal malignancies were retrieved. A total of 14 cases exhibited complete SMARCB1 (INI1) loss and glandular differentiation. SMARCA2 and SMARCA4 were normal, except for one case with a loss of SMARCA2. Next-generation sequencing (NGS) and/or fluorescence in situ hybridization (FISH) revealed an alteration in the SMARCB1 gene in 9/13 cases, while 2/13 were negative. Two tumors harbored SMARCB1 mutations in c.157C > T p.(Arg53Ter) and c.842G > A p.(Trp281Ter). One harbored ARID1B mutations in c.1469G > A p.(Trp490Ter) and MGA c.3724C > T p.(Arg1242Ter). Seven tumors had a SMARCB1 deletion. One carried an ESR1 mutation in c.644-2A > T, and another carried a POLE mutation in c.352_374del p.(Ser118GlyfsTer78). One case had a PAX3 mutation in c.44del p.(Gly15AlafsTer95). Histomorphology of SMARCB1-deficient adenocarcinoma was oncocytoid/rhabdoid and glandular, solid, or trabecular in 9/14 cases. Two had basaloid/blue cytoplasm and one showed focal signet ring cells. Yolk sac tumor-like differentiation with Schiller-Duval-like bodies was seen in 6/14 cases, with 2 cases showing exclusively reticular-microcystic yolk sac pattern. Follow-up of a maximum of 26 months (median 10 months) was available for 8/14 patients. Distant metastasis to the lung, liver, mediastinum, bone, and/or retroperitoneum was seen in 4/8 cases. Locoregional failure was seen in 75% of patients, with 6/8 local recurrences and 3 cervical lymph node metastases. At the last follow-up, 5 of 8 (62%) patients had died of their disease 2 to 20 months after diagnosis (median 8.2 months), and 3 were alive with the disease. The original diagnosis was usually high-grade non-intestinal-type adenocarcinoma or high-grade myoepithelial carcinoma. A correct diagnosis of these aggressive tumors could lead to improved targeted therapies with potentially better overall disease-specific survival.
650    _2
$a lidé $7 D006801
650    12
$a gen SMARCB1 $x nedostatek $x genetika $7 D000071796
650    _2
$a lidé středního věku $7 D008875
650    _2
$a mužské pohlaví $7 D008297
650    _2
$a ženské pohlaví $7 D005260
650    _2
$a senioři $7 D000368
650    12
$a adenokarcinom $x genetika $x patologie $7 D000230
650    _2
$a dospělí $7 D000328
650    12
$a transkripční faktory $x genetika $x nedostatek $7 D014157
650    12
$a myoepiteliální nádor $x genetika $x patologie $7 D009208
650    12
$a nádory vedlejších dutin nosních $x genetika $x patologie $7 D010255
650    12
$a mutace $7 D009154
650    _2
$a nádorové biomarkery $x genetika $7 D014408
650    _2
$a DNA vazebné proteiny $x genetika $x nedostatek $7 D004268
650    _2
$a hybridizace in situ fluorescenční $7 D017404
650    _2
$a diferenciální diagnóza $7 D003937
650    _2
$a senioři nad 80 let $7 D000369
650    _2
$a vysoce účinné nukleotidové sekvenování $7 D059014
650    _2
$a stupeň nádoru $7 D060787
655    _2
$a časopisecké články $7 D016428
700    1_
$a Taheri, Touraj $u Department of Anatomical Pathology, Queensland Health, Royal Brisbane and Women Hospital, University of Queensland, Brisbane, Australia
700    1_
$a Bradová, Martina $u Department of Pathology, Faculty of Medicine in Pilsen, Charles University, E. Benese 13, 305 99, Pilsen, Czech Republic $u Bioptic Laboratory, Ltd., Pilsen, Czech Republic
700    1_
$a Vaněček, Tomáš $u Molecular and Genetic Laboratory, Bioptic Laboratory, Ltd, Pilsen, Czech Republic
700    1_
$a Franchi, Alessandro $u Department of Translational Research, School of Medicine, University of Pisa, Pisa, Italy
700    1_
$a Slouka, David $u Department of Otorhinolaryngology, University Hospital in Pilsen, Faculty of Medicine in Pilsen, Charles University, Pilsen, Czech Republic
700    1_
$a Kostlivý, Tomáš $u Department of Otorhinolaryngology, University Hospital in Pilsen, Faculty of Medicine in Pilsen, Charles University, Pilsen, Czech Republic
700    1_
$a de Rezende, Gisele $u Department of Anatomic Histopathology and Cytogenetics, Department of Laboratory Medicine, Niguarda Cancer Center, Milan, Italy
700    1_
$a Michálek, Jaroslav $u Department of Clinical and Molecular Pathology, University Hospital and Medical Faculty of Palacky University, Olomouc, Czech Republic
700    1_
$a Klubíčková, Natálie $u Department of Pathology, Faculty of Medicine in Pilsen, Charles University, E. Benese 13, 305 99, Pilsen, Czech Republic $u Bioptic Laboratory, Ltd., Pilsen, Czech Republic
700    1_
$a Ptáková, Nicola $u Molecular and Genetic Laboratory, Bioptic Laboratory, Ltd, Pilsen, Czech Republic
700    1_
$a Nemcová, Antónia $u Pathological Laboratories, Medicyt, Ltd., Košice, Slovak Republic
700    1_
$a Michal, Michal $u Department of Pathology, Faculty of Medicine in Pilsen, Charles University, E. Benese 13, 305 99, Pilsen, Czech Republic $u Bioptic Laboratory, Ltd., Pilsen, Czech Republic
700    1_
$a Agaimy, Abbas $u Institute of Pathology, University Hospital Erlangen, Friedrich-Alexander University Erlangen-Nürnberg (FAU), Erlangen, Germany
700    1_
$a Leivo, Ilmo $u Institute of Biomedicine, Pathology, University of Turku and Department of Pathology, Turku University Hospital, Turku, Finland
773    0_
$w MED00004660 $t Virchows Archiv : an international journal of pathology $x 1432-2307 $g Roč. 485, č. 2 (2024), s. 245-256
856    41
$u https://pubmed.ncbi.nlm.nih.gov/38085333 $y Pubmed
910    __
$a ABA008 $b sig $c sign $y - $z 0
990    __
$a 20241015 $b ABA008
991    __
$a 20241024110611 $b ABA008
999    __
$a ok $b bmc $g 2202078 $s 1231599
BAS    __
$a 3
BAS    __
$a PreBMC-MEDLINE
BMC    __
$a 2024 $b 485 $c 2 $d 245-256 $e 20231212 $i 1432-2307 $m Virchows Archiv : an international journal of pathology $n Virchows Arch $x MED00004660
LZP    __
$a Pubmed-20241015

Find record

Citation metrics

Archiving options