Exploring macrophage cell therapy on Diabetic Kidney Disease

Guiteras, Roser; Solà, Anna; Flaquer, Maria; Manonelles, Anna; Hotter, Georgina; Cruzado, Josep M.

doi:10.1111/jcmm.13983

Cited by 27 publications

(22 citation statements)

References 56 publications

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“…Similar to this study, it has been found that NGAL KO mice had worse renal damage after IR-induced AKI [86]. Furthermore, NGAL therapy is effective in DN [87]. In this study, macrophage NGAL cell therapy increased the anti-inflammatory molecule IL-10 and decreased the proinflammatory molecule TNF-α, indicating that NGAL overexpressing macrophage therapy could reduce inflammation in DN.…”

Section: Macrophages Phenotype Under the Control Of Bioactive Moleculsupporting

confidence: 85%

Macrophage Phenotype and Fibrosis in Diabetic Nephropathy

Calle

Hotter

2020

IJMS

Self Cite

137

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Diabetic nephropathy (DN) is the leading cause of end-stage renal disease globally. The primary initiating mechanism in DN is hyperglycemia-induced vascular dysfunction, but its progression is due to different pathological mechanisms, including oxidative stress, inflammatory cells infiltration, inflammation and fibrosis. Macrophages (Mφ) accumulation in kidneys correlates strongly with serum creatinine, interstitial myofibroblast accumulation and interstitial fibrosis scores. However, whether or not Mφ polarization is involved in the progression of DN has not been adequately defined. The prevalence of the different phenotypes during the course of DN, the existence of hybrid phenotypes and the plasticity of these cells depending of the environment have led to inconclusive results. In the same sense the role of the different macrophage phenotype in fibrosis associated or not to DN warrants additional investigation into Mφ polarization and its role in fibrosis. Due to the association between fibrosis and the progressive decline of renal function in DN, and the role of the different phenotypes of Mφ in fibrosis, in this review we examine the role of macrophage phenotype control in DN and highlight the potential factors contributing to phenotype change and injury or repair in DN.

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Section: Macrophages Phenotype Under the Control Of Bioactive Moleculsupporting

confidence: 85%

Macrophage Phenotype and Fibrosis in Diabetic Nephropathy

Calle

Hotter

2020

IJMS

Self Cite

137

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“…Previous studies also have confirmed that the phagocytic activity of M2 Mφ is more efficient than that of M1 cells. 52,53 They attributed this to the higher activity of M2 Mφ in scavenging debris and tissue remodeling. 54,55 Furthermore, following hypoxia incubation of RAW264.7 cells for 24 h, CLU expression was enhanced (Figure 3), but those of the M1 marker CD80 and the M2 marker CD206 decreased, while the phagocytosis was also increased (data not shown).…”

Section: Clu Is Associated With Decreased Polarization To M1 After LImentioning

confidence: 99%

Clusterin regulates macrophage expansion, polarization and phagocytic activity in response to inflammation in the kidneys

Wang

Zhao

Guan

et al. 2020

Immunol. Cell Biol.

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Clusterin (CLU) is a multifunctional protein localized extracellularly and intracellularly. Although CLU-knockout (KO) mice are more susceptible to renal ischemia-reperfusion injury (IRI), the mechanisms underlying the actions of CLU in IRI are not fully understood. Macrophages are key regulators of IRI severity and tissue repair. Therefore, we investigated the role of CLU in macrophage polarization and phagocytosis. Renal IRI was induced in wild-type (WT) or CLU-KO C57BL/6 mice by clamping the renal pedicles for 30 min at 32°C. Peritoneal macrophages were activated via an intraperitoneal injection of lipopolysaccharide (LPS). Renal tissue damage was examined using histology, whereas leukocyte phenotypes were assessed using flow cytometry and immunohistochemistry. We found that monocytes/macrophages expressed the CLU protein that was upregulated by hypoxia. The percentages of macrophages (F4/80 + , CD11b + or MAC3 +) infiltrating the kidneys of WT mice were significantly less than those in CLU-KO mice after IRI. The M1/M2 phenotype ratio of the macrophages in WT kidneys decreased at day 7 post-IRI when the injury was repaired, whereas that in KO kidneys increased consistently as tissue injury persisted. In response to LPS stimulation, WT mice produced fewer M1 macrophages, but not M2, than the control did. Phagocytosis was stimulated by CLU expression in macrophages compared with the CLU null controls and by the exogenous CLU protein. In conclusion, CLU suppresses macrophage infiltration and proinflammatory M1 polarization during the recovery period following IRI, and enhances phagocytic activity, which may be partly responsible for tissue repair in the kidneys of WT mice after injury.

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“…We already demonstrated that cell therapy with modified macrophages ameliorate kidney damage in different experimental renal pathologies by decreasing the inflammatory scenario 5 – 7 . Given the properties of Ivns1abp-macrophages in actin cytoskeleton stability and the resistance against inflammatory insults, we therefore investigated whether cell therapy with these modified macrophages preserve kidney function and epithelial integrity against the inflammatory damage associated with I/R injury.…”

Section: Resultsmentioning

confidence: 99%

“…Lastly, given the properties of macrophages overexpressing Ivns1abp in actin cytoskeleton stability and resistance to inflammation and following our previous experience in cellular therapy with macrophages in renal pathology 5 – 7 , we hypothesized that these macrophages could be used as a treatment for damage associated with I/R injury. The experiments revealed that BMDMs that overexpress Ivns1abp were highly protective of renal function as well as the epithelial structure of renal tubules preventing mismatches of actin cytoskeleton loss.…”

Section: Discussionmentioning

confidence: 99%

“…Latter investigations suggest that targeting macrophage activation and phenotype can lead to new therapies in the treatment of acute and chronic diseases such as obesity, insulin resistance or asthma 3 , 4 . Along the same lines, our group has demonstrated the therapeutic effect of macrophage-cell therapy in different chronic and acute kidney diseases 5 – 7 .…”

Section: Introductionmentioning

confidence: 87%

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The influenza virus NS1A binding protein gene modulates macrophages response to cytokines and phagocytic potential in inflammation

Hotter

Mastora

Jung

et al. 2020

Sci Rep

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Macrophages show remarkable phenotypic plasticity in response to environmental signals. Although it is generally less considered, cytoskeletal changes in macrophages influence their phenotype, including phagocytosis and secretion of soluble cytokines. Influenza virus NS1A-binding protein (Ivns1abp) belongs to the Kelch family of proteins that play a central role in actin cytoskeleton dynamics by directly associating with F-actin and by protecting against actin derangement. Due to its role in cytoskeleton preservation, the Ivns1abp gene might be a critical regulator of the macrophage phenotype and function under inflammatory conditions. In this study, we determine that the modulation of the Ivns1abp gene in macrophages could modify resistance to macrophages against inflammation and maintain functional phagocytosis. Our results indicate that inflammatory insults inhibit the Ivns1abp gene, whereby phagocytosis is inhibited and the ability of macrophages to induce proliferation and repair of damaged cells is compromised. Furthermore, our results show that inflammatory insults alter the activity of the transcription factor c-myc, a factor which directly modulates the expression of the Ivns1abp gene. In conclusion, this study demonstrates a central role of lvns1abp in promoting and preserving a reparative macrophage phenotype and resistance to this inflammatory environment.

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Exploring macrophage cell therapy on Diabetic Kidney Disease

Cited by 27 publications

References 56 publications

Macrophage Phenotype and Fibrosis in Diabetic Nephropathy

Macrophage Phenotype and Fibrosis in Diabetic Nephropathy

Clusterin regulates macrophage expansion, polarization and phagocytic activity in response to inflammation in the kidneys

The influenza virus NS1A binding protein gene modulates macrophages response to cytokines and phagocytic potential in inflammation

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