Literature DB >> 29241742

Diagnostic utility of histone H3.3 G34W, G34R, and G34V mutant-specific antibodies for giant cell tumors of bone.

Hidetaka Yamamoto1, Takeshi Iwasaki2, Yuichi Yamada2, Yoshihiro Matsumoto3, Hiroshi Otsuka2, Masato Yoshimoto2, Kenichi Kohashi2, Kenichi Taguchi4, Ryohei Yokoyama5, Yasuharu Nakashima3, Yoshinao Oda2.   

Abstract

Giant cell tumors of bone (GCTBs) are characterized by mononuclear stromal cells and osteoclast-like giant cells; up to 95% have H3F3A gene mutation. The RANKL inhibitor denosumab, when used for the treatment of GCTB, leads to histological changes such as new bone formation and giant cell depletion. Here we assessed the diagnostic utility of immunohistochemical staining with the antibodies against histone H3.3 G34W, G34R and G34V mutant proteins for GCTB and other histologically similar bone and joint lesions. H3.3 G34W, G34R and G34V expressions were detected in mononuclear stromal cells in 47/51 (92%), 1/51 (2%) and 3/51 (6%) cases of primary GCTBs, respectively, in a mutually exclusive manner. All recurrent/metastatic GCTBs (n=14), post-denosumab GCTBs (n=8) and secondary malignant GCTBs (n=2) were positive for H3.3 G34W. The immunohistochemical results were essentially correlated with the H3F3A genotype determined by mutation analysis. In post-denosumab GCTBs, H3.3 G34W expression was seen in immature bone-forming cells. H3.3 G34W, G34R and G34V were negative in 121/122 cases of non-GCTB, including chondroblastoma, osteosarcoma, primary aneurysmal bone cyst and other giant cell-rich lesions. The exception was a single case of undifferentiated high-grade pleomorphic sarcoma that was positive for H3.3 G34W, suggesting the possibility of sarcomatous overgrowth of primary malignant GCTB. Therefore, H3.3 G34W/R/V mutant-specific antibodies are useful surrogate markers for the H3F3A genotype and helpful for the diagnosis of GCTB and its variants. The expression of H3.3 G34W mutant protein in post-denosumab GCTB suggests that neoplastic stromal cells may play a role in new bone formation.
Copyright © 2017 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Denosumab; Giant cell tumor of bone; H3F3A; Immunohistochemistry; Mutation

Mesh:

Substances:

Year:  2017        PMID: 29241742     DOI: 10.1016/j.humpath.2017.11.020

Source DB:  PubMed          Journal:  Hum Pathol        ISSN: 0046-8177            Impact factor:   3.466


  25 in total

Review 1.  Integration of denosumab therapy in the management of giant cell tumors of bone.

Authors:  Daniel T Miles; Ryan T Voskuil; Wood Dale; Joel L Mayerson; Thomas J Scharschmidt
Journal:  J Orthop       Date:  2020-03-28

Review 2.  Histone H3.3 mutation in giant cell tumor of bone: an update in pathology.

Authors:  Hidetaka Yamamoto; Shin Ishihara; Yu Toda; Yoshinao Oda
Journal:  Med Mol Morphol       Date:  2019-11-20       Impact factor: 2.309

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Journal:  Cancer Cytopathol       Date:  2018-05-14       Impact factor: 5.284

5.  H3F3A G34 mutation DNA sequencing and G34W immunohistochemistry analysis in 366 cases of giant cell tumors of bone and other bone tumors.

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Review 7.  Malignant giant cell tumour of bone: a review of clinical, pathological and imaging features.

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9.  Evaluating H3F3A K27M and G34R/V somatic mutations in a cohort of pediatric brain tumors of different and rare histologies.

Authors:  Vinicius Fernandes Oliveira; Graziella Ribeiro De Sousa; Antonio Carlos Dos Santos; Fabiano Pinto Saggioro; Helio Rubens Machado; Ricardo Santos de Oliveira; Luiz Gonzaga Tone; Elvis Terci Valera
Journal:  Childs Nerv Syst       Date:  2020-08-07       Impact factor: 1.475

10.  Recurrent novel HMGA2-NCOR2 fusions characterize a subset of keratin-positive giant cell-rich soft tissue tumors.

Authors:  Andrew L Folpe; Kemal Kösemehmetoğlu; Abbas Agaimy; Michael Michal; Robert Stoehr; Fulvia Ferrazzi; Pavel Fabian; Michal Michal; Alessandro Franchi; Florian Haller
Journal:  Mod Pathol       Date:  2021-03-19       Impact factor: 7.842

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