Severely impaired CTL killing is a feature of the neurological disorder Niemann-Pick disease type C1

Castiblanco, D; Rudd-Schmidt, JA; Noori, T; Sutton, VR; Hung, YH; Flinsenberg, TWH; Hodel, AW; Young, ND; Smith, N; Bratkovic, D; Peters, H; Walterfang, M; Trapani, JA; Brennan, AJ; Voskoboinik, I

Author(s): Castiblanco, D; Rudd-Schmidt, JA; Noori, T; Sutton, VR; Hung, YH; Flinsenberg, TWH; Hodel, AW; Young, ND; Smith, N; Bratkovic, D; Peters, H; Walterfang, M; Trapani, JA; Brennan, AJ; Voskoboinik, I;
Details: Publication Year 2022-03-24,Volume 139,Issue #12,Page 1833-1849
Journal Title: Blood
Publication Type: Research article
Abstract: Niemann-Pick disease type C1 (NP-C1) is a rare lysosomal storage disorder resulting from mutations in an endolysosomal cholesterol transporter, NPC1. Despite typically presenting with pronounced neurological manifestations, NP-C1 also resembles long-term congenital immunodeficiencies that arise from impairment of cytotoxic T lymphocyte (CTL) effector function. CTLs kill their targets through exocytosis of the contents of lysosome-like secretory cytotoxic granules (CGs) that store and ultimately release the essential pore-forming protein perforin and proapoptotic serine proteases, granzymes, into the synapse formed between the CTL and target cell. We discovered that NPC1 deficiency increases CG lipid burden, impairs autophagic flux through stalled trafficking of the transcription factor EB (TFEB), and dramatically reduces CTL cytotoxicity. Using a variety of immunological and cell biological techniques, we found that the cytotoxic defect arises specifically from impaired perforin pore formation. We demonstrated defects of CTL function of varying severity in patients with NP-C1, with the greatest losses of function associated with the most florid and/or earliest disease presentations. Remarkably, perforin function and CTL cytotoxicity were restored in vitro by promoting lipid clearance with therapeutic 2-hydroxypropyl-beta-cyclodextrin; however, restoration of autophagy through TFEB overexpression was ineffective. Overall, our study revealed that NPC1 deficiency has a deleterious impact on CTL (but not natural killer cell) cytotoxicity that, in the long term, may predispose patients with NP-C1 to atypical infections and impaired immune surveillance more generally.
Keywords: Cholesterol/metabolism; Granzymes; Humans; *Niemann-Pick Disease, Type A; *Niemann-Pick Disease, Type C/metabolism; Perforin/genetics; T-Lymphocytes, Cytotoxic/metabolism
Department(s): Laboratory Research
PubMed ID: 35081253
Publisher's Version: https://doi.org/10.1182/blood.2021013477
Terms of Use/Rights Notice: Refer to copyright notice on published article.

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