Stage-dependent immunity orchestrates AQP4 antibody-guided NMOSD pathology: a role for netting neutrophils with resident memory T cells in situ.

Nakajima, Akihiro; Yanagimura, Fumihiro; Saji, Etsuji; Shimizu, Hiroshi; Toyoshima, Yasuko; Yanagawa, Kaori; Arakawa, Musashi; Hokari, Mariko; Yokoseki, Akiko; Wakasugi, Takahiro; Okamoto, Kouichirou; Takebayashi, Hirohide; Fujii, Chihiro; Itoh, Kyoko; Takei, Yo-Ichi; Ohara, Shinji; Yamada, Mitsunori; Takahashi, Hitoshi; Nishizawa, Masatoyo; Igarashi, Hironaka; Kakita, Akiyoshi; Onodera, Osamu; Kawachi, Izumi

Nakajima, Akihiro; Yanagimura, Fumihiro; Saji, Etsuji; Shimizu, Hiroshi; Toyoshima, Yasuko; Yanagawa, Kaori; Arakawa, Musashi; Hokari, Mariko; Yokoseki, Akiko; Wakasugi, Takahiro; Okamoto, Kouichirou; Takebayashi, Hirohide; Fujii, Chihiro; Itoh, Kyoko; Takei, Yo-Ichi; Ohara, Shinji; Yamada, Mitsunori; Takahashi, Hitoshi; Nishizawa, Masatoyo; Igarashi, Hironaka; Kakita, Akiyoshi; Onodera, Osamu; Kawachi, Izumi.

Affiliation

Nakajima A; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Yanagimura F; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Saji E; Department of Neurology, NHO Niigata National Hospital, 3-52 Akasakamachi, Kashiwazaki, Niigata, 945-8585, Japan.
Shimizu H; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Toyoshima Y; Department of Pathology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Yanagawa K; Department of Pathology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Arakawa M; Department of Neurology, Brain Disease Center, Agano Hospital, 6317-15 Yasuda, Agano, Niigata, 959-2221, Japan.
Hokari M; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Yokoseki A; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Wakasugi T; Musashi Clinic, 20-1 Hakusanura 2, Chuo-Ku, Niigata, 951-8131, Japan.
Okamoto K; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Takebayashi H; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Fujii C; Department of Neurology, Niigata Medical Center, 27-11 Kobari 3, Nishi-Ku, Niigata, 950-2022, Japan.
Itoh K; Department of Neurology, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Takei YI; Department of Neurology, NHO Nishiniigata Chuo Hospital, 14-1 Masago 1, Nishi-Ku, Niigata, 950-2085, Japan.
Ohara S; Department of Neurosurgery, Brain Research Institute, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8585, Japan.
Yamada M; Division of Neurobiology and Anatomy, Graduate School of Medical and Dental Sciences, Niigata University, 1-757 Asahimachi, Chuo-Ku, Niigata, 951-8510, Japan.
Takahashi H; Department of Neurology, Kansai Medical University Medical Center, 10-15 Fumizonocho, Moriguchi, Osaka, 570-8507, Japan.
Nishizawa M; Department of Neurology, Graduate School of Medical Sciences, Kyoto Prefectural University of Medicine, 465 Kajii-Cho, Kawaramachi-Hirokoji, Kamigyo-Ku, Kyoto, 602-8566, Japan.
Igarashi H; Department of Pathology and Applied Neurobiology, Graduate School of Medical Sciences, Kyoto Prefectural University of Medicine, 465 Kajii-Cho, Kawaramachi-Hirokoji, Kamigyo-Ku, Kyoto, 602-8566, Japan.
Kakita A; Department of Neurology, NHO Matsumoto Medical Center, 2-20-30 Muraimachi-Minami, Matsumoto, Nagano, 399-8701, Japan.
Onodera O; Department of Neurology, NHO Matsumoto Medical Center, 2-20-30 Muraimachi-Minami, Matsumoto, Nagano, 399-8701, Japan.
Kawachi I; Department of Neurology, Iida Hospital, 1-15 Odori, Iida, Nagano, 395-8505, Japan.

Acta Neuropathol ; 147(1): 76, 2024 04 24.

Article in En | MEDLINE | ID: mdl-38658413

ABSTRACT

ABSTRACT

Neuromyelitis optica spectrum disorder (NMOSD) is an autoimmune disease of the CNS characterized by the production of disease-specific autoantibodies against aquaporin-4 (AQP4) water channels. Animal model studies suggest that anti-AQP4 antibodies cause a loss of AQP4-expressing astrocytes, primarily via complement-dependent cytotoxicity. Nonetheless, several aspects of the disease remain unclear, including how anti-AQP4 antibodies cross the blood-brain barrier from the periphery to the CNS; how NMOSD expands into longitudinally extensive transverse myelitis or optic neuritis; how multiphasic courses occur; and how to prevent attacks without depleting circulating anti-AQP4 antibodies, especially when employing B-cell-depleting therapies. To address these knowledge gaps, we conducted a comprehensive 'stage-dependent' investigation of immune cell elements in situ in human NMOSD lesions, based on neuropathological techniques for autopsied/biopsied CNS materials. The present study provided three major findings. First, activated or netting neutrophils and melanoma cell adhesion molecule-positive (MCAM+) helper T (TH) 17/cytotoxic T (TC) 17 cells are prominent, and the numbers of these correlate with the size of NMOSD lesions in the initial or early-active stages. Second, forkhead box P3-positive (FOXP3+) regulatory T (Treg) cells are recruited to NMOSD lesions during the initial, early-active or late-active stages, suggesting rapid suppression of proinflammatory autoimmune events in the active stages of NMOSD. Third, compartmentalized resident memory immune cells, including CD103+ tissue-resident memory T (TRM) cells with long-lasting inflammatory potential, are detected under "standby" conditions in all stages. Furthermore, CD103+ TRM cells express high levels of granzyme B/perforin-1 in the initial or early-active stages of NMOSD in situ. We infer that stage-dependent compartmentalized immune traits orchestrate the pathology of anti-AQP4 antibody-guided NMOSD in situ. Our work further suggests that targeting activated/netting neutrophils, MCAM+ TH17/TC17 cells, and CD103+ TRM cells, as well as promoting the expansion of FOXP3+ Treg cells, may be effective in treating and preventing relapses of NMOSD.

Subject(s)

Aquaporin 4; Autoantibodies; Neuromyelitis Optica; Neutrophils; Neuromyelitis Optica/immunology; Neuromyelitis Optica/pathology; Aquaporin 4/immunology; Humans; Neutrophils/immunology; Neutrophils/pathology; Female; Autoantibodies/immunology; Male; Middle Aged; Immunologic Memory; Adult; Aged; Th17 Cells/immunology; Th17 Cells/pathology

Key words

Forkhead box P3-positive (FOXP3+) regulatory T cells; Melanoma cell adhesion molecule-positive (MCAM+) helper T 17 cells; Multiple sclerosis; Neuromyelitis optica spectrum disorder; Neutrophil extracellular DNA traps; Tissue-resident memory T cells

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Autoantibodies / Neuromyelitis Optica / Aquaporin 4 / Neutrophils Limits: Adult / Aged / Female / Humans / Male / Middle aged Language: En Journal: Acta Neuropathol Year: 2024 Document type: Article Affiliation country: Japan

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