Antagonism of TIM-1 blocks the development of disease in a humanized mouse model of allergic asthma

Sonar, Sanchaita Sriwal; Hsu, Yen-Ming; Conrad, Melanie L.; Majeau, Gerard R.; Kılıç, Ayşe; Garber, Ellen A.; Yan, Gao; Nwankwo, Chioma; Willer, G.; Dudda, Jan C.; Kim, Hellen; Bailly, Véronique; Pagenstecher, Axel; Rennert, Paul D.; Renz, Harald

doi:10.1172/jci39543

Cited by 43 publications

(43 citation statements)

References 43 publications

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“…Transfected HEK 293T cells were detached with 1ϫ PBS plus 5 mM EDTA 48 h after transfection, washed with 1ϫ PBS plus 5% FBS, and incubated for 1 h with goat polyclonal antisera specific to mTIM-1, TIM-1, TIM-3, or TIM-4 as indicated (R&D Systems) at a concentration of 4 g/ml. Alternatively, cells were incubated for 1 h with human TIM-1 specific mouse monoclonal antibodies (MAbs) ARD5 or AKG7 (4,18,19) as indicated at a concentration of 5 g/ml. Normal goat serum or purified mouse IgG2a (R&D Systems) were used as negative controls.…”

Section: Methodsmentioning

confidence: 99%

Characterizing Functional Domains for TIM-Mediated Enveloped Virus Entry

Moller-Tank

Albritton

Rennert³

et al. 2014

J Virol

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T-cell immunoglobulin and mucin domain 1 (TIM-1) and other TIM family members were recently identified as phosphatidylserine (PtdSer)-mediated virus entry-enhancing receptors (PVEERs). These proteins enhance entry of Ebola virus (EBOV) and other viruses by binding PtdSer on the viral envelope, concentrating virus on the cell surface, and promoting subsequent internalization. The PtdSer-binding activity of the immunoglobulin-like variable (IgV) domain is essential for both virus binding and internalization by TIM-1. However, TIM-3, whose IgV domain also binds PtdSer, does not effectively enhance virus entry, indicating that other domains of TIM proteins are functionally important. Here, we investigate the domains supporting enhancement of enveloped virus entry, thereby defining the features necessary for a functional PVEER. Using a variety of chimeras and deletion mutants, we found that in addition to a functional PtdSer-binding domain PVEERs require a stalk domain of sufficient length, containing sequences that promote an extended structure. Neither the cytoplasmic nor the transmembrane domain of TIM-1 is essential for enhancing virus entry, provided the protein is still plasma membrane bound. Based on these defined characteristics, we generated a mimic lacking TIM sequences and composed of annexin V, the mucin-like domain of ␣-dystroglycan, and a glycophosphatidylinositol anchor that functioned as a PVEER to enhance transduction of virions displaying Ebola, Chikungunya, Ross River, or Sindbis virus glycoproteins. This identification of the key features necessary for PtdSer-mediated enhancement of virus entry provides a basis for more effective recognition of unknown PVEERs. IMPORTANCE T-cell immunoglobulin and mucin domain 1 (TIM-1) and other TIM family members are recently identified phosphatidylserine (PtdSer)-mediated virus entry-enhancing receptors (PVEERs). These proteins enhance virus entry by binding the phospholipid,PtdSer, present on the viral membrane. While it is known that the PtdSer binding is essential for the PVEER function of TIM-1, TIM-3 shares this binding activity but does not enhance virus entry. No comprehensive studies have been done to characterize the other domains of TIM-1. In this study, using a variety of chimeric proteins and deletion mutants, we define the features necessary for a functional PVEER. With these features in mind, we generated a TIM-1 mimic using functionally similar domains from other proteins. This mimic, like TIM-1, effectively enhanced transduction. These studies provide insight into the key features necessary for PVEERs and will allow for more effective identification of unknown PVEERs. T-cell immunoglobulin and mucin domain 1 (TIM-1; also called HAVCR-1, TIMD1, or KIM-1) is a member of the TIM family of type 1 cell surface glycoproteins. TIM-1 enhances entry of a broad range of viruses, including members of the picornavirus, filovirus, flavivirus, alphavirus, arenavirus, and baculovirus families (1-6). Although TIM-4 is less extensively studied, all eviden...

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Section: Methodsmentioning

confidence: 99%

Characterizing Functional Domains for TIM-Mediated Enveloped Virus Entry

Moller-Tank

Albritton

Rennert³

et al. 2014

J Virol

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“…Kim-1 is a member of the immunoglobulin family and is expressed in the surface of activated T cells (CD4 + Th2) (32); therefore, sKim-1 may be involved in the immune response to sepsis and its level is higher than normal in this condition. Previous animal and clinical studies have demonstrated (33,34) that Kim-1 is an inflammation mediator associated with the pathogenesis of asthma and rheumatoid arthritis. A prospective, multicenter cohort study (35) found that Kim-1 peaked at 2 days after cardiac surgery in adults and at 1 day after surgery in children, and that the elevations of Kim-1 were associated with AKI and adverse outcomes in adults.…”

Section: Group a (N=17) Group B (N=21) ------------------------------mentioning

confidence: 99%

Effect of continuous renal replacement therapy on kidney injury molecule-1 and neutrophil gelatinase-associated lipocalin in patients with septic acute kidney injury

Shao

Fan

Yin

et al. 2017

Experimental and Therapeutic Medicine

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Abstract. Kidney injury molecule-1 (Kim-1) and neutrophil gelatinase-associated lipocalin (NGAL) have been investigated as biomarkers for acute kidney injury (AKI). However, they are seldom investigated in patients with septic AKI treated with continuous renal replacement therapy (CRRT). The aim of the present study was to investigate the therapeutic effectiveness and possible mechanisms of CRRT in septic AKI by observing the changes in Kim-1 and NGAL levels. A group of 38 patients with septic AKI was randomly divided into the conventional drug treatment group (group A) and the CRRT group (group B). All patients were treated with standard antisepsis agents, and group B was additionally submitted to CRRT for 24 h. The levels of Kim-1 and NGAL in serum, urine and the ultrafiltrate of CRRT were measured prior to and at 12, 24, and 48 h after treatment. In group A, urinary Kim-1 (uKim-1) levels at 12, 24 and 48 h were lower than prior to treatment (P<0.05), whereas urinary NGAL (uNGAL) showed no difference among the various time points (P>0.05). In group B, uKim-1 was decreased at 24 and 48 h compared with before treatment (all P<0.05), whereas uNGAL was decreased at 48 h (P<0.05). Serum Kim-1 did not change with time in groups A and B (P>0.05), whereas serum NGAL was increased after treatment in group A (P<0.05) but did not change in group B (P>0.05). Kim-1 and NGAL were not detected in the ultrafiltrate of CRRT. uKim-1 and uNGAL decreased significantly after CRRT, and therefore may be used to reflect the change of renal function during CRRT and to evaluate the therapeutic effectiveness of the method.

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“…Anti‐TIM‐1 antibody (Clone RMT1‐10) ameliorates Experimental autoimmune encephalomyelitis (EAE),17 allergic asthma,37 glomerulonephritis38 and corneal allograft rejection 39. In contrast another anti‐TIM‐1 antibody (clone 3B3) enhances T cell proliferation and Th2 effector function 17, 40, 41.…”

Section: Discussionmentioning

confidence: 99%

Anti‐TIM‐1 Monoclonal Antibody (RMT1‐10) Attenuates Atherosclerosis By Expanding IgM‐producing B1a Cells

Hosseini

Kanellakis

et al. 2018

JAHA

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BackgroundPeritoneal B1a cells attenuate atherosclerosis by secreting natural polyclonal immunoglobulin M (IgM). Regulatory B cells expressing T‐cell immunoglobulin mucin domain‐1 (TIM‐1) expanded through TIM‐1 ligation by anti‐TIM‐1 monoclonal antibody (RMT1‐10) induces immune tolerance.Methods and ResultsWe examined the capacity of RMT1‐10 to expand peritoneal B1a cells to prevent atherosclerosis development and retard progression of established atherosclerosis. RMT1‐10 treatment selectively doubled peritoneal B1a cells, tripled TIM‐1+ B1a cells and increased TIM‐1+IgM+interleukin (IL)‐10+ by 3‐fold and TIM‐1+IgM+IL‐10− B1a cells by 2.5‐fold. Similar expansion of B1a B cells was observed in spleens. These effects reduced atherosclerotic lesion size, increased plasma IgM and lesion IgM deposits, and decreased oxidatively modified low‐density lipoproteins in lesions. Lesion CD4+ and CD8+ T cells, macrophages and monocyte chemoattractant protein‐1, vascular cell adhesion molecule‐1, expression of proinflammatory cytokines monocyte chemoattractant protein‐1, vascular cell adhesion molecule‐1, IL1β, apoptotic cell numbers and necrotic cores were also reduced. RMT1‐10 treatment failed to expand peritoneal B1a cells and reduce atherosclerosis after splenectomy that reduces B1a cells, indicating that these effects are B1a cell‐dependent. Apolipoprotein E‐KO mice fed a high‐fat diet for 6 weeks before treatment with RMT1‐10 also increased TIM‐1+IgM+ IL‐10+ and TIM‐1+IgM+ IL‐10− B1a cells and IgM levels and attenuated progression of established atherosclerosis.Conclusions RMT1‐10 treatment attenuates atherosclerosis development and progression by selectively expanding IgM producing atheroprotective B1a cells. Antibody‐based in vivo expansion of B1a cells could be an attractive approach for treating atherosclerosis.

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Antagonism of TIM-1 blocks the development of disease in a humanized mouse model of allergic asthma

Cited by 43 publications

References 43 publications

Characterizing Functional Domains for TIM-Mediated Enveloped Virus Entry

Characterizing Functional Domains for TIM-Mediated Enveloped Virus Entry

Effect of continuous renal replacement therapy on kidney injury molecule-1 and neutrophil gelatinase-associated lipocalin in patients with septic acute kidney injury

Anti‐TIM‐1 Monoclonal Antibody (RMT1‐10) Attenuates Atherosclerosis By Expanding IgM‐producing B1a Cells

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