Histiocytic and Dendritic Cell Sarcomas of Hematopoietic Origin Share Targetable Genomic Alterations Distinct from Follicular Dendritic Cell Sarcoma

Lucas R Massoth; Yin P Hung; Judith A Ferry; Robert P Hasserjian; Valentina Nardi; G Petur Nielsen; Sam Sadigh; Vinayak Venkataraman; Martin Selig; Alison M Friedmann; Wesley Samore; Jonathan Keith Killian; Riza Milante; Joseph Giessinger; Kathleen Foley-Peres; Chelsea Marcus; Eric Severson; Daniel Duncan; Smruthy Sivakumar; Jeffrey S Ross; Vikram Desphande; Shakti H Ramkissoon; Jo-Anne Vergilio; Abner Louissaint; Lawrence R Zukerberg; Erik A Williams

doi:10.1002/onco.13801

Histiocytic and Dendritic Cell Sarcomas of Hematopoietic Origin Share Targetable Genomic Alterations Distinct from Follicular Dendritic Cell Sarcoma

Oncologist. 2021 Jul;26(7):e1263-e1272. doi: 10.1002/onco.13801. Epub 2021 May 6.

Authors

Lucas R Massoth^#¹, Yin P Hung^#¹, Judith A Ferry¹, Robert P Hasserjian¹, Valentina Nardi¹, G Petur Nielsen¹, Sam Sadigh², Vinayak Venkataraman^{3

4}, Martin Selig¹, Alison M Friedmann³, Wesley Samore¹, Jonathan Keith Killian⁵, Riza Milante⁶, Joseph Giessinger⁷, Kathleen Foley-Peres⁸, Chelsea Marcus⁵, Eric Severson⁵, Daniel Duncan⁵, Smruthy Sivakumar⁵, Jeffrey S Ross^{5

9}, Vikram Desphande¹, Shakti H Ramkissoon^{5

10}, Jo-Anne Vergilio⁵, Abner Louissaint¹, Lawrence R Zukerberg^#¹, Erik A Williams^#^{5

11}

Affiliations

¹ Department of Pathology, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts, USA.
² Department of Pathology, Brigham and Women's Hospital and Harvard Medical School, Boston, Massachusetts, USA.
³ Department of Pediatrics, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts, USA.
⁴ Department of Medicine, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts, USA.
⁵ Foundation Medicine, Inc., Cambridge, Massachusetts, USA.
⁶ Department of Dermatology, Jose R. Reyes Memorial Medical Center, Manila, Philippines.
⁷ A.T. Still University School of Osteopathic Medicine, Mesa, Arizona, USA.
⁸ Department of Biology, Bristol Community College, Fall River, Massachusetts, USA.
⁹ Department of Pathology, State University of New York Upstate Medical University, Syracuse, New York, USA.
¹⁰ Wake Forest Comprehensive Cancer Center and Department of Pathology, Wake Forest School of Medicine, Winston-Salem, North Carolina, USA.
¹¹ Department of Pathology, Department of Dermatology, UCSF Dermatopathology Service, University of California San Francisco, San Francisco, California, USA.

^# Contributed equally.

Abstract

Background: Histiocytic and dendritic cell neoplasms are a diverse group of tumors arising from monocytic or dendritic cell lineage. Whereas the genomic features for Langerhans cell histiocytosis and Erdheim-Chester disease have been well described, other less common and often aggressive tumors in this broad category remain poorly characterized, and comparison studies across the World Health Organization diagnostic categories are lacking.

Methods: Tumor samples from a total of 102 patient cases within four major subtypes of malignant histiocytic and dendritic cell neoplasms, including 44 follicular dendritic cell sarcomas (FDCSs), 41 histiocytic sarcomas (HSs), 7 interdigitating dendritic cell sarcomas (IDCSs), and 10 Langerhans cell sarcomas (LCSs), underwent hybridization capture with analysis of up to 406 cancer-related genes.

Results: Among the entire cohort of 102 patients, CDKN2A mutations were most frequent across subtypes and made up 32% of cases, followed by TP53 mutations (22%). Mitogen-activated protein kinase (MAPK) pathway mutations were present and enriched among the malignant histiocytosis (M) group (HS, IDCS, and LCS) but absent in FDCS (72% vs. 0%; p < .0001). In contrast, NF-κB pathway mutations were frequent in FDCSs but rare in M group histiocytoses (61% vs. 12%; p < .0001). Tumor mutational burden was significantly higher in M group histiocytoses as compared with FDCSs (median 4.0/Mb vs. 2.4/Mb; p = .012). We also describe a pediatric patient with recurrent secondary histiocytic sarcoma treated with targeted therapy and interrogated by molecular analysis to identify mechanisms of therapeutic resistance.

Conclusion: A total of 42 patient tumors (41%) harbored pathogenic mutations that were potentially targetable by approved and/or investigative therapies. Our findings highlight the potential value of molecular testing to enable precise tumor classification, identify candidate oncogenic drivers, and define personalized therapeutic options for patients with these aggressive tumors.

Implications for practice: This study presents comprehensive genomic profiling results on 102 patient cases within four major subtypes of malignant histiocytic and dendritic cell neoplasms, including 44 follicular dendritic cell sarcomas (FDCSs), 41 histiocytic sarcomas (HSs), 7 interdigitating dendritic cell sarcomas (IDCSs), and 10 Langerhans cell sarcomas (LCSs). MAPK pathway mutations were present and enriched among the malignant histiocytosis (M) group (HS, IDCS, and LCS) but absent in FDCSs. In contrast, NF-κB pathway mutations were frequent in FDCSs but rare in M group histiocytosis. A total of 42 patient tumors (41%) harbored pathogenic mutations that were potentially targetable by approved and/or investigative therapies.

Keywords: Follicular dendritic cell sarcoma; Histiocytic sarcoma; Interdigitating dendritic cell sarcoma; Malignant histiocytosis; Targeted therapy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Child
Dendritic Cell Sarcoma, Follicular* / genetics
Dendritic Cells
Genomics
Hematopoietic Stem Cell Transplantation*
Humans
Mutation
Neoplasm Recurrence, Local
Sarcoma* / genetics