Generalised reduction of putative endothelial progenitors and CXCR4-positive peripheral blood cells in type 2 diabetes

Egan, Colin Gerard; Lavery, Rowena; Caporali, Francesca; Fondelli, Cecilia; Laghi-Pasini, Franco; Dotta, Francesco; Sorrentino, Vincenzo

doi:10.1007/s00125-008-0939-6

Cited by 113 publications

(92 citation statements)

References 49 publications

(77 reference statements)

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“…In this issue of Diabetologia, Egan et al provide further demonstration of a reduction in EPC levels in unselected type 2 diabetic patients [4]. To understand why another confirmatory study was needed, we have to take a few steps backwards, because this hot topic has prompted broad discussion on ways of identifying and isolating the bloodderived progenitors [5].…”

mentioning

confidence: 99%

An underlying principle for the study of circulating progenitor cells in diabetes and its complications

Fadini

2008

Diabetologia

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mentioning

confidence: 99%

An underlying principle for the study of circulating progenitor cells in diabetes and its complications

Fadini

2008

Diabetologia

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“…The cells expressing CXCR4 correlates positively with the progenitor cells amount on normal individual, while on diabetic patients, there is no correlation. Other research indicated that there is significant decrease of CXCR4 expression in PBMC of type 2 diabetic patients [24]. The decrease of circulated EPC amount is affected by the low ability of EPC cells in responding to SDF-1 [36].…”

Section: Flow Cytometric Analysis Of Sdf-1 Relative Amountmentioning

confidence: 95%

“…Although without complication, the amount of progenitor cells majority on diabetic patients still significantly lower than healthy control. The endothelial progenitor cells reduction can also be happened on patients with high blood glucose level and HbA 1c (glycated hemoglobin) [24]. The previous research mentioned that the amount of CD34 + , one type of the immature cell which was circulated in blood and becomes the part of endothelial progenitor cells (EPC), was lower in diabetic b a a a a…”

Section: Flow Cytometric Analysis Of Cd34 + Relative Amountmentioning

confidence: 99%

Detection of VipAlbumin® Effect in CD34 and SDF-1 Mobilization, in Streptozotocin-induced Diabetes Mellitus Mice

Pradana

Djati

Rifa’i

2015

JELS

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Diabetes mellitus is a disease in which the body loses its ability to provide tight regulation and maintain a dynamic interaction between the tissue sensitivity and insulin secretion by β cells. The impact of this dysfunctional mechanism is uncontrolled blood glucose levels that lead to hyperglycemia condition. Highly reactive free radicals have a strong involvement in the pathogenesis of diabetes mellitus, where one of its forming process may be triggered by hyperglycemia condition. Patients with diabetes mellitus itself vulnerable to endothelial dysfunction, which is caused by a decrease in circulating endothelial progenitor cells, and also a decrease in chemokines which play a role in affecting the activities of these cells. Hyperglycemia condition and free radical activity is a major cause of these endothelial progenitor cells dysfunction.The purpose of this study was to determine the role of VipAlbumin®, a supplement derived from Channa striatus albumin extracts in inhibiting the action of free radicals that are formed due to hyperglycemia condition, which can affect the increase in endothelial progenitor cells relative amount. This study used BALB/C mice that induced to undergo diabetes mellitus through streptozotocin injection intraperitoneally at 5-day old. Mice who have reached 4 week old and positive to diabetes mellitus (blood glucose levels > 200 mg.dl -1 ) will be administered with VipAlbumin® orally for 14 days. VipAlbumin® dosage was divided into 4 groups: positive control (without VipAlbumin®); 1 st dose (0.01664 mg.gr -1 BW); 2 nd dose (0.416 mg.gr -1 BW); 3 rd dose (10.4 mg.gr -1 BW). The last step was flow cytometric analysis to determine the development of endothelial progenitor cells relative amount, which isolated from bone marrow. The variables measured in this study were the relative amount of CD34 + and SDF-1. Based to flow cytometric analysis, mice with VipAlbumin® administration did not show any significant improvement in CD34 relative amount when compared to the positive control. Relative amount of Chemokine SDF-1 itself, although only occur at the 3 rd dose of VipAlbumin® treatment, has increased and significantly different from the positive control.

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“…It was reported the presence in PB of a stem cell population which lack the CD34 antigen and is able to differentiate into CD34+CD133+ EPCs, and acquire a more mature endothelial phenotype (Friedrich et al, 2006). Additionally, other populations with endothelial repair capabilities which express additional cell surface markers, including the receptor for SDF-1, the chemokine (C-X-C motif) receptor (CXCR)-4 have also been identified (Egan et al, 2008). The characterization of these different subpopulations of EPCs is due to the different methodology used for cell isolation.…”

Section: Epcs Phenotypic and Functional Propertiesmentioning

confidence: 99%

“…Additionally, several subsets of EPCs have been identified and together with other lineages of precursor cells were found to be differentially recruited to neovascular foci contributing synergistically to vasculogenic neoformation (Gulati et al, 2003;Hur et al, 2004;Lyden et al, 2001;Yoon et al, 2005a). Since their identification, an increasing body of evidence has definitely revealed the important properties and roles played by EPCs in several vascularrelated diseases, such as peripheral vascular disease (Asahara et al, 1999a(Asahara et al, , 1999bTakahashi et al, 1999), tumor neovascularisation (Asahara et al, 1999a(Asahara et al, , 1999bLyden et al, 2001) and vascular complications associated to diabetes (Goon et al, 2007;Grant et al, 2002;Egan et al, 2008;Fadini et al, 2005). The metabolic alterations present in diabetic individuals are known to profoundly affect vascular biology, being responsible for the impairment of macro-and microvascular beds (Fadini et al, 2006a;Werner et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

Vasculogenesis in Diabetes-Associated Diseases: Unraveling the Diabetic Paradox

Costa¹

2011

Vasculogenesis and Angiogenesis - From Embryonic Development to Regenerative Medicine

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Generalised reduction of putative endothelial progenitors and CXCR4-positive peripheral blood cells in type 2 diabetes

Cited by 113 publications

References 49 publications

An underlying principle for the study of circulating progenitor cells in diabetes and its complications

An underlying principle for the study of circulating progenitor cells in diabetes and its complications

Detection of VipAlbumin® Effect in CD34 and SDF-1 Mobilization, in Streptozotocin-induced Diabetes Mellitus Mice

Vasculogenesis in Diabetes-Associated Diseases: Unraveling the Diabetic Paradox

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