Ex vivo programmed macrophages ameliorate experimental chronic inflammatory renal disease

Wang, Y.; Wang, Y.P.; Zheng, Guoping; Lee, Vincent; Ouyang, Linqi; Chang, Dan; Mahajan, Deepika; Coombs, Jana; Wang, Y.M.; Alexander, Stephen I.; Harris, David C.H.

doi:10.1038/sj.ki.5002275

Cited by 328 publications

(311 citation statements)

References 47 publications

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“…In contrast, inhibition of nuclear factor-κB, a regulator of macrophage functional differentiation, reprogrammes macrophages so that they become profoundly anti-inflammatory in settings where they would normally be classically activated and attenuate glomerular inflammation in vivo [35]. Furthermore, ex vivo manipulation of macrophages using specific cytokines confirmed that classically activated, M1 macrophages worsen chronic inflammatory adriamycin nephropathy, whereas alternatively activated M2 macrophages reduce histological disruption and functional injury [36]. Of note, in the heart Camargo et al [37] have [39] Glycerol-induced ARF (mouse) MSCs Enhanced tubular proliferation [68] IR (rat) Papilla LRCs Proliferation and incorporation [149] IR (mouse) Bone marrow No functional improvement, intrarenal cells are the main source of repopulating cell during repair [22] Folic acid-induced acute tubular injury (mouse) Bone marrow Intrinsic tubular cell proliferation accounts for repair after damage [150] Folic acid-induced acute tubular injury (mouse) Bone marrow 10% incorporation in tubules and G-CSF doubles this rate [151] IR (rat) MSCs Improved renal function and less injury [152] Cisplatin-induced renal failure (mouse) MSCs Accelerated tubular proliferation [153] UUO (mouse) Bone marrow macrophages Reduced renal fibrosis [41] IR (rat) MSCs Improved renal function, increased proliferation and decreased apoptosis [84] IR (rat) rKS56 (S3 segment outgrowth) Replace tubular and improve function [80] Glycerol-induced tubulonecrosis (mouse) Human CD133 + cells Homing and tubular integration [66] UUO (rat) Label-retaining cells (LRC) Proliferates, migrates and transdifferentiates into fibroblast-like cells [27] Cisplatin-induced renal failure (mouse) G-CSF ± M-CSF Improvement in renal function and prevention of renal tubular injury [154] Anti-Thy1.1 GN (rat) MSCs Increased glomerular proliferation and reduction in proteinuria [53] Col4α3 deficiency (mouse) MSCs Prevented loss of peritubular capillaries and reduced fibrosis but no increase in function or survival [24] Col4α3 deficiency (mouse) Bone marrow Partial restoration of expression of the type IV collagen α3 chain, improved histology and function [25] Col4α3 deficiency (mouse) MSCs Improved function and glomerular scarring and interstitial fibrosis reduced [155] UUO (mouse) BM Instertitial BM-derived cells do not contribute significantly to collagen synthesis after damage [74] Adriamycin-nephropathy (mo...…”

Section: Bone Marrow-derived Cellsmentioning

confidence: 96%

Stem cell options for kidney disease

Hopkins

Rae

et al. 2008

The Journal of Pathology

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Chronic kidney disease (CKD) is increasing at the rate of 6-8% per annum in the US alone. At present, dialysis and transplantation remain the only treatment options. However, there is hope that stem cells and regenerative medicine may provide additional regenerative options for kidney disease. Such new treatments might involve induction of repair using endogenous or exogenous stem cells or the reprogramming of the organ to reinitiate development. This review addresses the current state of understanding with respect to the ability of non-renal stem cell sources to influence renal repair, the existence of endogenous renal stem cells and the biology of normal renal repair in response to damage. Understanding repair options via an understanding of renal developmentThe prevalence and incidence of chronic kidney disease (CKD) is increasing at 6-8% per annum in the USA alone, largely as a result of increased prevalence of diabetes and obesity [1]. To understand what might be possible with respect to cellular therapies or regenerative medicine for the kidney, one first needs to consider what is understood about normal renal development and response to injury. The kidney has been classically regarded as an organ with minimal cellular turnover and no capacity for regeneration. The subsequent identification of stem cells in a number of such organs, including the brain, has challenged this view. However, the dogma remains that the kidney reaches a maximal complement of nephrons and then loses these over time [2]. This dogma is drawn from our understanding of the development of this organ. The progenitor population during developmentThe kidney is mesodermal in origin and develops from two populations derived from intermediate mesoderm, the ureteric bud (UB) and the metanephric mesenchyme (MM). While an even broader potential had been proposed [3], genetic and lineage analyses have confirmed that the MM gives rise to all portions of the nephron other than the collecting ducts and also gives rise to elements of the renal interstitium [4][5][6]. The UB gives rise to the ureter and collecting ducts only. The MM is apparently not homogeneous but forms condensed mesenchyme around the tips of the branching UB. This cap mesenchyme (CM) contains self-renewing progenitors capable of generating all cells of the nephron other than the collecting ducts via an initial mesenchyme-epithelial transition (MET) event throughout the prenatal developmental period [6]. The continued expression of the transcription factor Six2 in CM is required for maintenance of this stem cell population during kidney development [5]. As the UB branches and extends through the MM, individual MET events occur at the underside of each tip to form a new nephron [2]. This nephron endowment therefore proceeds from the centre of the kidney out to the periphery, with the CM stem cell field remaining on the outer edge of the expanding organ. Endowment of new nephrons is restricted to prenatal development in humans, while in rodents it persists only until the imm...

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Section: Bone Marrow-derived Cellsmentioning

confidence: 96%

Stem cell options for kidney disease

Hopkins

Rae

et al. 2008

The Journal of Pathology

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“…Macrophages exhibiting this AAM phenotype were found in the lung later than 100 days post infection (data not shown). A number of differences in chemokine expression have been described between classical and alternatively activated macrophages [13][14][15]. To further characterize the Mac3 hi CD11b hi hemosiderin-laden macrophages, we assessed CCL5, CXCL11 and CCL17 chemokine expression levels in sorted cells.…”

Section: Long-term Hemorrhaging and Alternative Macrophage Activationmentioning

confidence: 99%

Nippostrongylus brasiliensis infection leads to the development of emphysema associated with the induction of alternatively activated macrophages

et al. 2008

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Chronic obstructive pulmonary disease (COPD) is the 5 th most prevalent disease worldwide leading to severe morbidity and mortality in developed countries. The disease is strongly associated with smoking, and can be characterized by progressive and irreversible deterioration in lung function and destruction of the lung parenchyma. We show here that infection with the hookworm Nippostrongylus brasiliensis results in deterioration in lung function, destruction of alveoli and long-term airways hyperresponsiveness, consistent with COPD and emphysema. N. brasiliensis infection leads to chronic low level hemorrhaging in the lung and the presence of hemosiderinladen macrophages in the absence of an overt inflammatory infiltrate. Microarray analysis of gene expression in diseased lungs and quantitative RT-PCR analysis of purified macrophages revealed a state of prolonged tissue injury and the presence of alternatively activated macrophages producing MMP-12. Taken together, these data show that lung tissue damage caused by hookworm infection can result in the development of COPD and emphysema.

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“…Les macrophages M1, délétères, produisent des radicaux libres oxygénés et sécrètent des cytokines pro-inflammatoires telles que le TNF- et l'IL-1-. Ces produits étant toxiques pour les cellules résidentes rénales, ils contribuent ainsi à l'extension des lésions et à la progression de la fibrose (Figure 2) [6,7]. À l'inverse, les macrophages de type M2 exercent un rôle protecteur.…”

Section: Phase D'apparition Des Myofibroblastes : Un Pour Tous Tousunclassified

“…À l'inverse, les macrophages de type M2 exercent un rôle protecteur. En effet, bien qu'ils soient capables de produire du TGF- et de la MEC, phénomènes qui a priori sont associés à un effet pro-fibrosant, leur rôle principal est de réduire l'inflammation grâce à la sécrétion de cytokines antiinflammatoires comme l'IL-10 et l'IL-6 ( Figure 2) [6,7]. Ainsi Wang et al ont mis en évidence que le transfert de macrophages polarisés (Figure 1) [11].…”

Section: Phase D'apparition Des Myofibroblastes : Un Pour Tous Tousunclassified

“…Dans cette revue, nous analyserons donc quels sont les mécanismes et les facteurs de progression de la FTI et quelles sont les stratégies thérapeutiques envisageables pour l'avenir. < ex vivo vers un phénotype M2 permettait de réduire l'inflammation et le développement de la fibrose rénale chez l'animal alors que le transfert de macrophages de type M1 aggravait les lésions [7]. Bien que les macrophages soient toujours reconnus comme étant les acteurs-clés de l'inflammation associée à la FTI, il est donc désormais nécessaire de mieux caractériser le rôle relatif de ces deux populations.…”

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La fibrose tubulo-interstitielle rénale

Klein

Miravète²,

Buffin-Meyer³

et al. 2011

Med Sci (Paris)

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La fibrose rénale : un problème de santé publique L'évolution de nos sociétés et de nos modes de vie, l'augmentation de l'incidence de l'obésité, des maladies cardiovasculaires, du diabète, ainsi que le vieillissement de la population entraînent l'accroissement exponentiel du nombre de patients atteints de maladies rénales chroniques et évoluant à plus ou moins long terme vers l'insuffisance rénale terminale. À ce stade, les patients sont soignés par des thérapies de remplacement lourdes et coûteuses comme la dialyse et la transplantation. Bien que les causes primitives des atteintes rénales soient multiples, la majorité des néphropathies évo-luent vers le développement d'une fibrose rénale. La fibrose est définie par une accumulation exagérée de matrice extracellulaire (MEC) [41]. Elle peut se déve-lopper dans de nombreux organes (peau, foie, poumons, coeur, rein) et sa présence est souvent associée à la perte de la fonction de l'organe touché. Au niveau rénal, il existe trois grands types de fibrose, dépendant de l'étiologie de la maladie : la fibrose vasculaire, la fibrose glomérulaire (ou glomérulosclérose) et la fibrose tubulo-interstitielle (FTI). À l'heure actuelle, la majorité des maladies rénales chroniques ont pour > Le vieillissement de la population et l'augmentation du nombre de patients atteints de diabète entraînent une forte accélération de l'incidence des néphropathies menant à l'insuffisance rénale. Quelle qu'en soit l'origine, la majorité des atteintes rénales aboutissent au développement d'une fibrose tubulo-interstitielle (FTI) dont la présence signe l'évolution vers la perte de la fonction rénale. Comprendre et lutter contre le développe-ment de la FTI représente ainsi un enjeu scientifique et médical de la plus grande importance. Dans cette revue, nous analyserons donc quels sont les mécanismes et les facteurs de progression de la FTI et quelles sont les stratégies thérapeutiques envisageables pour l'avenir. < origine une atteinte glomérulaire et sont donc associées à des lésions de glomérulosclérose. Cependant, la fibrose progresse ensuite presque toujours vers le compartiment tubulo-interstitiel [1] ; d'un point de vue clinique, la présence de FTI est fortement corrélée à une future évolution vers l'insuffisance rénale et est ainsi associée à un mauvais pronostic à long terme [2]. Pour toutes ces raisons, le développement de la FTI, qui fut pendant longtemps une menace silencieuse, est sur le point de devenir un problème majeur de santé publique et ce, au niveau mondial. Au cours des dernières années, de grands efforts de recherche ont ainsi été entrepris afin de mieux comprendre les mécanismes de la FTI et de pouvoir, un jour, développer de nouvelles stratégies thérapeutiques et entrer en guerre contre cette maladie. La trilogie de la fibrose rénaleLa FTI est un processus complexe, qui implique de nombreuses molé-cules et de nombreux types cellulaires, résidents ou infiltrés. Il est possible de diviser de manière schématique le développement de la FTI en trois phases distinctes : la pha...

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Ex vivo programmed macrophages ameliorate experimental chronic inflammatory renal disease

Cited by 328 publications

References 47 publications

Stem cell options for kidney disease

Stem cell options for kidney disease

Nippostrongylus brasiliensis infection leads to the development of emphysema associated with the induction of alternatively activated macrophages

La fibrose tubulo-interstitielle rénale

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