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POS0340 EFFECTS OF CAR-T CELL TREATMENT ON B CELL IMMUNITY IN SYSTEMIC AUTOIMMUNE DISEASES

免疫 细胞免疫 细胞 免疫学 B细胞 医学 免疫系统 生物 抗体 遗传学
作者
L. Bucci,T. Rothe,Fabian Müller,J. Taubmann,Melanie Hagen,C. Bergmann,Carlo Tur,Luis E. Muñoz,Alexander Wilhelm,R. Gerlach,Sebastian Schäfer,S. Völkl,M. Aigner,Ricardo Grieshaber‐Bouyer,G. Krönke,A. Bozec,Tobias Winkler,A. Mackensen,G. Schett
出处
期刊:Annals of the Rheumatic Diseases [BMJ]
标识
DOI:10.1136/annrheumdis-2024-eular.1519
摘要

Background:

Treatment with autologous CD19 chimeric antigen receptor (CAR) T cells induces deep depletion of B cells in humans. This potential may allow resetting aberrant B-cell immunity in patients with autoimmune diseases such as systemic lupus erythematosus (SLE), idiopathic inflammatory myositis (IIM) and systemic sclerosis (SSc).

Objectives:

To investigate the effects of CD19 CAR-T cell treatment on B cell immunity in patients with SLE, IIM and SSc.

Methods:

Spectral analyzer-based characterization of B cell subsets in 8 SLE, 2 IIM and 2 SSc patients at baseline, early reconstitution (EaR) 4 months and established reconstitution (EsR) one year after CD19 CAR-T cell therapy. High-throughput single-cell mRNA sequencing of B cells with an Illumina NovaSeq platform in 5 SLE patients before and one year after CD19 CAR-T cell therapy. VH repertoire analysis of B cells based on VDJ library preparation and Illumina MiSeq sequencing in each one patient with SLE, IIM and SSc one year after CD19 CAR-T cell therapy and comparison with VH repertoire of two healthy controls.

Results:

Characterization of B cell subsets revealed that reconstituted B cells at EaR and EsR showed a naïve phenotype, while CD19+CD27+ memory B cells were drastically reduced. A limited increase in CD19+CD27+ memory B cells occurred between EaR and EsR, which was predominantly seen in pre-switched IgD+ CD27+ B cells. CD27+CD38+ plasmablasts and SLE-associated activated CD11c+ memory B cells disappeared in SLE patients after B cell reconstitution. Immature CD38+ B cells, indicating reconstitution of B cells from the bone marrow boosted at EaR and declined thereafter. Similar results were also seen in at EaR an EsR of B cells in IIM and SSc. Single cell sequencing-based analysis of heavy chains in SLE patients showed virtual disappearance of IGHG1, IGHG2, IGHG3, IGHG4, IGHA1 and IGHA2 chains, while the expression of IGHM and IGHD increased, resembling a non-class switched B cell receptor phenotype. The expression of distinct chains associated with SLE and autoimmunity, such as immunoglobulin kappa variable (IGKV) 4-1, immunoglobulin heavy variable (IGHV) 4-59 chain and immunoglobulin lambda variable (IGLV) 3-21 chain was downregulated. In addition, a broad and balanced VH – JH usage was found in SLE, IIM and SSc patients treated with CAR-T cells without any noticeable clonal expansions, very similar to a normal B cell repertoire of naïve B cells from healthy controls. Analysis of the frequency of somatic mutations in the VH genes revealed that all IgM sequences had a very low mutation frequency similar to a repertoire from sorted naïve cells from healthy controls.

Conclusion:

Altogether the appearance of a naïve non-class-switched B cell system, the disappearance of circulating plasmablasts, the down regulation of specific disease- associated heavy and light chains and the broad and balanced VH – JH usage support the concept that CD19 CAR-T cell therapy may have induced a reset of pathologic B cell autoimmunity in patients with systemic autoimmune disease.

REFERENCES:

[1] Mougiakakos D et al., CD19-Targeted CAR T Cells in Refractory Systemic Lupus Erythematosus. N Engl J Med 2021;385:567-569. [2] Mackensen A. et al., Anti-CD19 CAR T cell therapy for refractory systemic lupus erythematosus; Nat Med 2022 Oct; 28(10):2124-2132.

Acknowledgements:

NIL.

Disclosure of Interests:

None declared.

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