NGFR regulates stromal cell activation in germinal centers.

Nerve growth factor receptor (NGFR) is expressed by follicular dendritic cells (FDCs). However, the role of NGFR in the humoral response is not well defined. Here, we study the effect of Ngfr loss on lymph node organization and function, demonstrating that Ngfr depletion leads to spontaneous germinal center (GC) formation and an expansion of the GC B cell compartment. In accordance with this effect, stromal cells are altered in Ngfr-/- mice with a higher frequency of FDCs, characterized by CD21/35, MAdCAM-1, and VCAM-1 overexpression. GCs are located ectopically in Ngfr-/- mice, with lost polarization together with impaired high-affinity antibody production and an increase in circulating autoantibodies. We observe higher levels of autoantibodies in Bcl2 Tg/Ngfr-/- mice, concomitant with a higher incidence of autoimmunity and lower overall survival. Our work shows that NGFR is involved in maintaining GC structure and function, participating in GC activation, antibody production, and immune tolerance.

Demultiplexing Ig repertoires by parallel mRNA/DNA sequencing shows major differential alterations in severe COVID-19.

To understand the fine differential elements that can lead to or prevent acute respiratory distress syndrome (ARDS) in COVID-19 patients, it is crucial to investigate the immune response architecture. We herein dissected the multiple layers of B cell responses by flow cytometry and Ig repertoire analysis from acute phase to recovery. Flow cytometry with FlowSOM analysis showed major changes associated with COVID-19 inflammation such as an increase of double-negative B-cells and ongoing plasma cell differentiation. This paralleled COVID-19-driven expansion of two disconnected B-cell repertoires. Demultiplexing successive DNA and RNA Ig repertoire patterns characterized an early expansion of IgG1 clonotypes with atypically long and uncharged CDR3, the abundance of this inflammatory repertoire being correlated with ARDS and likely pejorative. A superimposed convergent response included convergent anti-SARS-CoV-2 clonotypes. It featured progressively increasing somatic hypermutation together with normal-length or short CDR3 and it persisted until a quiescent memory B-cell stage after recovery.

[Perspectives for the evolution and use of CAR-T cells]. / Perspectives d'évolution et d'utilisation des cellules CAR-T.

CAR-T cells have recently made a stunning entry on the arena of immunotherapy of B-cell lymphomas. This new treatment approach represents the culmination of 30 years of efforts to understand the role of T cells in the antitumor response. However, this technology is still in its infancy and suffers from a number of limitations. Many areas for improvement, based in particular on the possibilities of additional genetic manipulations of CAR-T cells, aim at reducing their toxicity, increasing their persistence in vivo, preventing the risk of tumor escape, recruiting other immune effectors, or extending their application to other cancers. Further studies of the dynamic interaction between the patient and these live drugs will allow elucidating the mechanisms determining the antitumor response in this context and thus developing more efficiently the future CAR-T cells.

Characterization of the novel HLA-DQA1*05:13 allele by next-generation sequencing.

DQA1*05:13 differs from DQA1*05:05:01:04 by one nucleotide substitution at position 37 in exon 1.

Characterization of the novel HLA-DQA1*05:18 allele by next-generation sequencing.

DQA1*05:18 differs from DQA1*05:01:01:03 by one nucleotide substitution at position 94 in exon 2.

Characterization of the novel HLA-B*08:67:02N allele by next-generation sequencing.

HLA-B*08:67:02N differs from B*08:01:01:01 by one nucleotide substitution at position 224 in exon 2.

Characterization of the novel HLA-DQA1*03:11 allele by next-generation sequencing.

DQA1*03:11 differs from DQA1*03:03:01:01 by one nucleotide substitution at position 664 in exon 4.

Characterization of the novel HLA-DQA1*01:19 allele by next-generation sequencing.

DQA1*01:19 differs from DQA1*01:02:01:04 by one nucleotide substitution at position 731 in exon 4.

Characterization of the novel HLA-DRB1*11:260 allele by next-generation sequencing.

DRB1*11:260 differs from DRB1*11:03:01 by one nucleotide substitution at position 484 in exon 3.

Characterization of the novel HLA-DQB1*02:162N allele by next-generation sequencing.

DQB1*02:162N differs from DQB1*02:02:01:01 by one nucleotide substitution at position 276 in exon 2.

Characterization of the novel HLA-DQB1*03:417 allele by next-generation sequencing.

DQB1*03:417 differs from DQB1*03:01:01:01 by one nucleotide substitution at position 179 in exon 2.

Characterization of the novel HLA-B*44:476 allele by next-generation sequencing.

B*44:476 differs from B*44:03:01:01 by one nucleotide substitution at position 934 in exon 5.

Characterization of the novel HLA-DRB1*01:107 allele by next-generation sequencing.

DRB1*01:107 differs from DRB1*01:01:01:01 by one nucleotide substitution at position 484 in exon 3.

Characterization of the novel HLA-DRB1*08:97 allele by next-generation sequencing.

DRB1*08:97 differs from DRB1*08:03:02:01 by one nucleotide substitution at position 485 in exon 3.

Characterization of the novel HLA-B*44:452 allele by next-generation sequencing.

B*44:452 differs from B*44:02:01:01 by one nucleotide substitution at position 527 in exon 3.

Characterization of the novel HLA-B*07:384 allele by next-generation sequencing.

B*07:384 differs from B*07:02:01:01 by one nucleotide substitution at position 472 in exon 3.

Characterization of the novel HLA-B*35:460Q allele by next-generation sequencing.

B*35:460Q differs from B*35:03:01:01 by one nucleotide substitution at position 406 in exon 3.