Immunohistochemical analysis of 147 cases of low-grade endometrial stromal sarcoma: refining the immunohistochemical profile of LG-ESS on a large, molecularly confirmed series

Low-grade endometrial stromal sarcoma (LG-ESS) can present diagnostic challenges, due to its overlapping morphological features with other uterine mesenchymal tumors. Misdiagnosis rates remain significant, and immunohistochemical data for LG-ESS are limited to small series and inconsistent antibody...

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Veröffentlicht in:Virchows Archiv : an international journal of pathology 2025-01
Hauptverfasser: Flídrová, Miroslava, Dundr, Pavel, Vránková, Romana, Němejcová, Kristýna, Cibula, David, Poncová, Renata, Michalová, Květoslava, Bouda, Jiří, Laco, Jan, Ndukwe, Munachiso, Ryś, Janusz, Książek, Mariusz, Berjon, Alberto, Zapardiel, Ignacio, Franin, Ivan, Njavro, Antonela, Hausnerová, Jitka, Bretová, Petra, Židlík, Vladimír, Klát, Jaroslav, Krasznai, Zoard Tibor, Poka, Robert, Volodko, Nataliya, Yezhova, Iryna, Pilka, Radovan, Marek, Radim, Kolnikova, Georgina, Krkoška, Milan, Halaška, Michael, Drozenová, Jana, Dolinská, Dagmar, Kalist, Vladimír, Bobiński, Marcin, Ostrowska-Leśko, Marta, Bizoń, Magdalena, Sawicki, Włodzimierz, Stukan, Maciej, Grabowska, Karolina, Jędryka, Marcin, Poprawski, Tymoteusz, Stolnicu, Simona, Căpîlna, Mihai Emil, Špůrková, Zuzana, Zikán, Michal, Ciccarone, Francesca, Scambia, Giovanni, Sharashenidze, Archil, Gudadze, Miranda, Piatnytska, Tetiana, Varchak, Ihor, Kendall Bártů, Michaela
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Sprache:eng
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Zusammenfassung:Low-grade endometrial stromal sarcoma (LG-ESS) can present diagnostic challenges, due to its overlapping morphological features with other uterine mesenchymal tumors. Misdiagnosis rates remain significant, and immunohistochemical data for LG-ESS are limited to small series and inconsistent antibody panels. This study aimed to refine the IHC profile of LG-ESS by analyzing a large, molecularly confirmed series of 147 cases using a panel of 24 antibodies, including newer markers like transgelin and smoothelin. CD10 and IFITM1, key endometrial stromal markers, were expressed in 86% (92% of those extensively) and 69% (60% of those extensively) of cases, with fusion-positive tumors showing significantly higher expression. Smooth muscle markers (α-SMA, desmin, h-caldesmon, calponin, transgelin) were variably expressed, predominantly in focal or low-intensity patterns, with α-SMA reaching the highest frequency of expression (44%). However, the intensity of smooth muscle marker expression was usually very low. Smoothelin was rarely expressed. Hormone receptors were frequently positive, with PR showing a higher frequency (92% vs. 83%) and intensity than ER. Markers like S-100, HMB45, and CD117 were largely negative; all tumors were p53 wild-type, with preserved SMARCB1/SMARCA4 expression and ALK and ROS1 negativity. This work represents the largest molecularly validated IHC study on LG-ESS, providing a robust diagnostic profile for routine pathology. By addressing key diagnostic limitations and examining newer markers, our study supports a more standardized approach to diagnosing LG-ESS and underscores the value of immunohistochemical panels, particularly in fusion-negative tumors where diagnosis relies on morphological and immunohistochemical interpretation. These findings contribute critical data for improving diagnostic accuracy.
ISSN:0945-6317
1432-2307
1432-2307
DOI:10.1007/s00428-025-04026-4