Anti-complement 5 antibody ameliorates antibody-mediated rejection after liver transplantation in rats

Tajima, Tetsuya; Hata, Koichiro; Kusakabe, Jiro; Miyauchi, Hidetaka; Badshah, Joshua Sam; Kageyama, Shoichi; Zhao, Xiangdong; Kim, Sung-Kwon; Tsuruyama, Tatsuaki; Kirchner, Varvara A.; Watanabe, Takeshi; Üemoto, Shinji; Hatano, Etsuro

doi:10.3389/fimmu.2023.1186653

Cited by 21 publications

(2 citation statements)

References 58 publications

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“…Likewise, the molecular phenotype of cABMR was associated with genes of fibrogenesis, and histological features of lobular hepatitis and liver fibrosis by a correlation with the HAI and with the LAF score. Of note, in a rat model of ABMR after LT DEGs enriched in pathways of TNF-signaling via NF-κB were more abundant in ABMR 36 .…”

Section: Discussionmentioning

confidence: 92%

Molecular signatures of chronic antibody-mediated rejection in human liver transplants

Engel,

Alaswad,

Campos-Murguia

et al. 2024

Preprint

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Background&Aims: The role of antibody-mediated rejection (ABMR) after liver transplantation (LT) remains controversial. Chronic ABMR (cABMR) is often subclinical and potentially missed without surveillance biopsies (svLbx) which are not established in most LT centers. Transcriptome analysis previously characterized molecular changes in T cell-mediated rejection (TCMR) after solid organ transplantation. We aimed to identify molecular cABMR signatures after LT for a more comprehensive understanding of cABMR. Methods: We retrospectively identified indication and svLbx from our prospective institutional biorepository (n=1207 over 12 years). We performed RNA-sequencing on liver biopsies (discovery cohort: n=71; validation cohort: n=58). Downstream analyses explored the unique and common molecular features of cABMR, clinical (clinTCMR) and subclinical TCMR (subTCMR) compared to no histological rejection (NHR). Results: Nineteen percent of LT recipients with donor-specific antibodies had cABMR. Eighty-one percent of patients with cABMR had ALT and AST ≤2x the upper limit of normal, only being recognized by svLbx. The cABMR group displayed differentially expressed genes (DEGs) uniquely enriched in fibrogenesis-, complement activation- and TNFα-signaling-related pathways. ClinTCMR showed DEGs uniquely enriched in antigen presentation-, interferon-signaling-, and T cell receptor-signaling-related pathways. Common cABMR and clinTCMR DEGs were enriched in chemokine-signaling- and cytokine response-related pathways. Gene set enrichment scores of interferon-signaling and extracellular matrix remodeling pathways discriminated cABMR and clinTCMR. Molecular signatures of clinTCMR correlated with histological TCMR-patterns. Molecular cABMR-signatures correlated with lobular graft injury and liver fibrosis scores. The validation cohort consistently showed patterns of DEGs associating cABMR with fibrogenesis- and NF-κB-signaling-related pathways and clinTCMR with interferon-signaling- and adaptive immunity-related pathways. SubTCMR was molecularly almost indistinguishable from NHR. Conclusions: We report transcriptome-unique features of cABMR that is a unique molecular identity associated with inflammation and fibrogenesis.

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Section: Discussionmentioning

confidence: 92%

Molecular signatures of chronic antibody-mediated rejection in human liver transplants

Engel,

Alaswad,

Campos-Murguia

et al. 2024

Preprint

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“…Interestingly, studies have shown that liver regeneration is dependent on complement. Complement C3 in the proliferative response could be independent of the C3a-C3aR interaction; instead, C3a and C5a appear to act through crosstalk with the local formation of cytokine networks, particularly IL-6 and TNF ( 177 , 355 ). In addition to complement and CRP, SAA also participates in liver-related diseases.…”

Section: Liver and Diseasesmentioning

confidence: 99%

Interorgan communication with the liver: novel mechanisms and therapeutic targets

Zhao,

Zhang,

et al. 2023

Front. Immunol.

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The liver is a multifunctional organ that plays crucial roles in numerous physiological processes, such as production of bile and proteins for blood plasma, regulation of blood levels of amino acids, processing of hemoglobin, clearance of metabolic waste, maintenance of glucose, etc. Therefore, the liver is essential for the homeostasis of organisms. With the development of research on the liver, there is growing concern about its effect on immune cells of innate and adaptive immunity. For example, the liver regulates the proliferation, differentiation, and effector functions of immune cells through various secreted proteins (also known as “hepatokines”). As a result, the liver is identified as an important regulator of the immune system. Furthermore, many diseases resulting from immune disorders are thought to be related to the dysfunction of the liver, including systemic lupus erythematosus, multiple sclerosis, and heart failure. Thus, the liver plays a role in remote immune regulation and is intricately linked with systemic immunity. This review provides a comprehensive overview of the liver remote regulation of the body’s innate and adaptive immunity regarding to main areas: immune-related molecules secreted by the liver and the liver-resident cells. Additionally, we assessed the influence of the liver on various facets of systemic immune-related diseases, offering insights into the clinical application of target therapies for liver immune regulation, as well as future developmental trends.

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Molecular mechanisms underlying the modulation of T-cell proliferation and cytotoxicity by immobilized CCL21 and ICAM1

Yado,

Dassa,

Zoabi

et al. 2024

Preprint

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A major challenge in adoptive cancer immunotherapy is the effective balance between the proliferation and cytotoxic capacity of effector CD8+ T cells. In this study, we explored the molecular mechanisms through which a "synthetic immune niche" (SIN), composed of immobilized CCL21 and ICAM1, modulates the interplay between these two cellular properties. Temporal phenotypic profiling of OVA-specific murine T cells revealed major differences in the response to SIN stimulation following antigen-specific and nonspecific activation. Thus, SIN treatment enhanced both the expansion and cytotoxicity of cells activated by OVA-loaded DCs on day 4, while similar treatment of cells activated by anti-CD3/CD28-conjugated beads dramatically enhanced cell expansion but unexpectedly blocked their cytotoxicity, which fully recovered only on day 7. Molecular profiling suggested that upregulation of cytotoxic gene signatures drives the SIN effect following DC activation, while downregulation of exhaustion and proapoptotic genes optimizes the proliferation-cytotoxicity balance in bead-activated cells.

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Anti-complement 5 antibody ameliorates antibody-mediated rejection after liver transplantation in rats

Cited by 21 publications

References 58 publications

Molecular signatures of chronic antibody-mediated rejection in human liver transplants

Molecular signatures of chronic antibody-mediated rejection in human liver transplants

Interorgan communication with the liver: novel mechanisms and therapeutic targets

Molecular mechanisms underlying the modulation of T-cell proliferation and cytotoxicity by immobilized CCL21 and ICAM1

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