Clinical characteristics and prognostic value of renal immune complex deposition in patients with light chain amyloidosis

Yan, Jipeng; Wang, Di; Jin, Zhao; Zhou, Meilan; Huang, Boyong; Xing, Yan; Guo, Wei-Feng; Sun, Shan

doi:10.3389/fonc.2022.949702

Cited by 1 publication

(2 citation statements)

References 40 publications

(41 reference statements)

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“…18 Furthermore, the mere conversion of free antibodies to adsorbed complexes instead results in granular or clump-like deposition of immune complexes and a rebound activation of the pro-inflammatory transcriptional profile of immune cells. 19 Therefore, the strategy that can adsorb across lineages and degrade DSA complexes to restore the single-cell transcriptional heterogeneity in an allograft is urgently needed. Disruption of single-cell transcriptional heterogeneity is an inevitable consequence of persistent multilineage DSA production and allosensitization.…”

Section: Introductionmentioning

confidence: 99%

“…Cell-membrane-coated nanoparticles, as a new type of nanocarrier, have shown considerable potential for clinical application especially with membrane protein genetic engineering, typically composed of a polymer core and a naturally derived outer layer of the cell membrane. , However, it is difficult to achieve the adsorption of multiple immunoglobulin types with a single engineering strategy due to the large span of DSA repertoires . Furthermore, the mere conversion of free antibodies to adsorbed complexes instead results in granular or clump-like deposition of immune complexes and a rebound activation of the pro-inflammatory transcriptional profile of immune cells . Therefore, the strategy that can adsorb across lineages and degrade DSA complexes to restore the single-cell transcriptional heterogeneity in an allograft is urgently needed.…”

Section: Introductionmentioning

confidence: 99%

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Single-Cell Heterogeneity Restorative Chimeric Engineering Nanoparticles for Alleviating Antibody-Mediated Allograft Injury

Lin

et al. 2023

ACS Appl. Mater. Interfaces

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Disturbance of single-cell transcriptional heterogeneity is an inevitable consequence of persistent donor-specific antibody (DSA) production and allosensitization. However, identifying and efficiently clearing allospecific antibody repertoires to restore single-cell transcriptional profiles remain challenging. Here, inspired by the high affinity of natural bacterial proteins for antibodies, a genetic engineered membrane-coated nanoparticle termed as DSA trapper by the engineering chimeric gene of protein A/G with phosphatidylserine ligands for macrophage phagocytosis was reported. It has been shown that DSA trappers adsorbed alloreactive antibodies with high saturation and activated the heterophagic clearance of antibody complexes, alleviating IgG deposition and complement activation. Remarkably, DSA trappers increased the endothelial protective lineages by 8.39-fold, reversed the highly biased cytotoxicity, and promoted the proliferative profiles of Treg cells, directly providing an obligate immune tolerant niche for single-cell heterogeneity restoration. In the mice of allogeneic transplantation, the DSA trapper spared endothelial from inflammatory degenerative rosette, improved the glomerular filtration rate, and prolonged the survival of allogeneic mice from 23.6 to 78.3 days. In general, by identifying the lineage characteristics of rejection-related antibodies, the chimeric engineered DSA trapper realized immunoadsorption and further phagocytosis of alloantibody complexes to restore the single-cell genetic architecture of the allograft, offering a promising prospect for the treatment of alloantibody-mediated immune injury.

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Section: Introductionmentioning

confidence: 99%