CD153/CD30 signaling promotes age-dependent tertiary lymphoid tissue expansion and kidney injury
Yuki Sato, … , Nagahiro Minato, Motoko Yanagita
Yuki Sato, … , Nagahiro Minato, Motoko Yanagita
Published November 23, 2021
Citation Information: J Clin Invest. 2022;132(2):e146071. https://doi.org/10.1172/JCI146071.
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Research Article Inflammation Nephrology Article has an altmetric score of 43

CD153/CD30 signaling promotes age-dependent tertiary lymphoid tissue expansion and kidney injury

Abstract

Tertiary lymphoid tissues (TLTs) facilitate local T and B cell interactions in chronically inflamed organs. However, the cells and molecular pathways that govern TLT formation are poorly defined. Here, we identified TNF superfamily CD153/CD30 signaling between 2 unique age-dependent lymphocyte subpopulations, CD153+PD-1+CD4+ senescence-associated T (SAT) cells and CD30+T-bet+ age-associated B cells (ABCs), as a driver for TLT expansion. SAT cells, which produced ABC-inducing factors IL-21 and IFN-γ, and ABCs progressively accumulated within TLTs in aged kidneys after injury. Notably, in kidney injury models, CD153 or CD30 deficiency impaired functional SAT cell induction, which resulted in reduced ABC numbers and attenuated TLT formation with improved inflammation, fibrosis, and renal function. Attenuated TLT formation after transplantation of CD153-deficient bone marrow further supported the importance of CD153 in immune cells. Clonal analysis revealed that SAT cells and ABCs in the kidneys arose from both local differentiation and recruitment from the spleen. In the synovium of aged rheumatoid arthritis patients, T peripheral helper/T follicular helper cells and ABCs also expressed CD153 and CD30, respectively. Together, our data reveal a previously unappreciated function of CD153/CD30 signaling in TLT formation and propose targeting the CD153/CD30 signaling pathway as a therapeutic target for slowing kidney disease progression.

Authors

Yuki Sato, Akiko Oguchi, Yuji Fukushima, Kyoko Masuda, Naoya Toriu, Keisuke Taniguchi, Takahisa Yoshikawa, Xiaotong Cui, Makiko Kondo, Takeshi Hosoi, Shota Komidori, Yoko Shimizu, Harumi Fujita, Li Jiang, Yingyi Kong, Takashi Yamanashi, Jun Seita, Takuya Yamamoto, Shinya Toyokuni, Yoko Hamazaki, Masakazu Hattori, Yasunobu Yoshikai, Peter Boor, Jürgen Floege, Hiroshi Kawamoto, Yasuhiro Murakawa, Nagahiro Minato, Motoko Yanagita

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Figure 8

Aged CD153–/– mice exhibit attenuated TLT formation with improved inflammation, fibrosis, and renal function in adenine nephropathy model.

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Aged CD153–/– mice exhibit attenuated TLT formation with improved inflam...
(A) Experimental protocol for BI (n = 4–9 at each time point). In 0.20% adenine nephropathy models, CD153-deficient (CD153–/–) mice exhibited defective TLT formation and attenuated renal dysfunction, inflammation, and fibrosis, as shown by (B) periodic acid–Schiff (PAS) staining, (C) serum creatinine (sCr) levels, (D) total TLT numbers, (E) advanced-stage TLT numbers, (F) PAS and Masson’s trichrome (MTC) staining, (G) tubular injury scores, (H) fibrosis scores, and (I) Cxcl13, Ccl19, Ifng, Tnfa, Col1a1, and Acta2 mRNA levels. Data are presented as mean ± SD. The yellow arrowheads in B indicate the localization of TLTs. Statistical significance was determined by an unpaired, 2-tailed t test. *P < 0.05; **P < 0.01; ***P < 0.001. Scale bars: 300 μm (B) and 100 μm (F).