Teclistamab induces rapid clinical response and deep tissue depletion in refractory systemic sclerosis-a case series
Authors
- Elise Siegert
- Elpida Phithak
- Fredrik N. Albach
- Robert Biesen
- Norman Michael Drzeniek
- Maria Dzamukova
- Isabell Haase
- Klaus Søndergaard
- Dorothea Schleser
- Leonard Fiebig
- Arne Sattler
- Ioanna Minopoulou
- Marie Chiara Rehm
- Phillip Kremer
- Udo Schneider
- Sofia Trezzini
- Anna Maria Claire Rein
- Clara Marisa Mayer
- Felix Doellinger
- Christian Furth
- Anja Staeck
- Qingyu Cheng
- Benedikt Sinzinger
- Nadine Unterwalder
- Sarah Ohrndorf
- Meike Probst
- Yaosi Li
- Daniel Grund
- Thula Walter-Rittel
- Anja Fleischmann
- Edgar Wiebe
- Marie Luise Hütter-Krönke
- Ulrich Keller
- Jan Krönke
- Antonia Busse
- Arnd Kleyer
- Ann-Christin Pecher
- Jörg Henes
- Anne Troldborg
- Anja Erika Hauser
- Ina Kötter
- Martin Krusche
- Gerhard Krönke
- Tobias Alexander
- David Simon
Journal
- Annals of the Rheumatic Diseases
Citation
- Ann Rheum Dis
Abstract
OBJECTIVES: This study aimed to evaluate clinical outcomes, serologic changes, and immunologic effects induced by the bispecific B cell Maturation Antigen (BCMA)x Cluster of Differentiation (CD)3 T-cell-engaging antibody teclistamab in systemic sclerosis (SSc). METHODS: Patients with severe and treatment-refractory SSc were treated with teclistamab as offlabel therapy. Blood and tissue samples from skin and bone marrow were analysed with immunohistochemistry and flow cytometry, serum antibodies were quantified by enzyme-linked immunosorbent assay (ELISA). Clinical efficacy was assessed using the American College of Rheumatology Composite Response Index in Systemic Sclerosis (ACR-CRISS) responses, among others. RESULTS: Ten patients with SSc (70% female; median age 51 years [IQR: 7]) completed 1 cycle of teclistamab. Two patients with advanced SSc heart involvement died shortly after treatment initiation. B-cells and plasma cells were almost completely eliminated from bone marrow and skin, accompanied by a median reduction of 70.6% (IQR: 39%) in antitopoisomerase antibody titres, decreases in serum IgG, and vaccination titres. After a median follow-up of 3.75 months (IQR: 2.5 months), 71% and 43% of patients achieved revised ACR-CRISS 25 and 50 responses, respectively. Among patients with interstitial lung disease, radiographic and functional improvement was observed by week 12 with a median increase in forced vital capacity of 7% (IQR: 15%). Skin fibrosis similarly improved, with a median decrease in the modified Rodnan skin score of 35.9% (IQR: 17.9%), accompanied by corresponding reductions in fibroblast activation protein (FAP)alpha-positive fibroblasts in skin biopsy specimens. CONCLUSIONS: Teclistamab induced deep tissue depletion of B-cells and plasma cells and rapid clinical and serological responses, with evidence for resolution of inflammation and potential modification of fibrotic processes. These data suggest the potential of BCMA-directed therapies to promote immune modulation and tissue remodelling.