Methods on LDL particle isolation, characterization, and component fractionation for the development of novel specific oxidized LDL status markers for atherosclerotic disease risk assessment

The present study uses simple, innovative methods to isolate, characterize and fractionate LDL in its main components for the study of specific oxidations on them that characterize oxidized low-density lipoprotein (oxLDL) status, as it causatively relates to atherosclerosis-associated cardiovascular disease (CVD) risk assessment. These methods are: (a) A simple, relatively time-short, low cost protocol for LDL isolation, to avoid shortcomings of the currently employed ultracentrifugation and affinity chromatography methodologies. (b) LDL purity verification by apoB100 SDS-PAGE analysis and by LDL particle size determination; the latter and its serum concentration are determined in the present study by a simple method more clinically feasible as marker of CVD risk assessment than nuclear magnetic resonance. (c) A protocol for LDL fractionation, for the first time, into its main protein/lipid components (apoB100, phospholipids, triglycerides, free cholesterol, and cholesteryl esters), as well as into LDL carotenoid/tocopherol content. (d) Protocols for the measurement, for the first time, of indicative specific LDL component oxidative modifications (cholesteryl ester-OOH, triglyceride-OOH, free cholesterol-OOH, phospholipid-OOH, apoB100-MDA, and apoB100-DiTyr) out of the many (known/unknown/under development) that collectively define oxLDL status, which contrasts with the current non-specific oxLDL status evaluation methods. The indicative oxLDL status markers, selected in the present study on the basis of expressing early oxidative stress-induced oxidative effects on LDL, are studied for the first time on patients with end stage kidney disease on maintenance hemodialysis, selected as an indicative model for atherosclerosis associated diseases. Isolating LDL and fractionating its protein and main lipid components, as well as its antioxidant arsenal comprised of carotenoids and tocopherols, paves the way for future studies to investigate all possible oxidative modifications responsible for turning LDL to oxLDL in association to their possible escaping from LDL’s internal antioxidant defense. This can lead to studies to identify those oxidative modifications of oxLDL (after their artificial generation on LDL), which are recognized by macrophages and convert them to foam cells, known to be responsible for the formation of atherosclerotic plaques that lead to the various CVDs

Markets of progression of renal injury in renal tissue and urine of patients with nephrotic syndrome

It is well established that albuminuria is an unfavorable prognostic factor for patients with various types of glomerulonephritis (GN), however, this is not observed in all patients. It is therefore important to identify more specific prognostic markers that reflect the healing process of injury or the progression to fibrosis. The aim of this study was to identify early markers of progression to renal injury in patients with significant degree of albuminuria.As such markers the expression of transgelin (SM22) and transglutaminase–2 (TG2) was studied. SM22 is expressed specifically in smooth muscle cells and is an early marker of epithelial to mesenchymal transition. TG–2 is an enzyme that contributes to renal scarring through altering extracellular matrix homeostasis.SM22 was studied in 67 patients with various kinds of GN and a 5 year follow up. SM22 was identified in kidney sections at the time of diagnosis using immunohistochemistry and immunofluorescence. SM22 expression was examined concerning its correlation with the clinical course of GNs. The expression of alpha smooth muscle actin (a–SMA) and co-localization with SM22 was also investigated. TG2 expression was studied by immunofluorescence in kidney sections from 32 patients with MN. These MN patients were subsequently treated by combination of cyclosporine and prednisolone for 24 months with a repeat biopsy taken in 14. Kidney sections from the normal part of kidneys were used as normal controls for the expression of the aforementioned molecules.Forty six out of 67 patients, that transgelin was studied, showed stable renal function. In control biopsies SM22 and a-SMA were restricted to vascular wall whereas in patients with GN expression was extended within glomeruli and the interstitium. SM22 expression correlated to the degree of glomerular sclerosis and interstitial fibrosis, to the degree of mesangial proliferation and renal function outcome. Double staining for co-localization of both SMM22 and a-SMA showed that in some areas of kidney tissue both proteins were identified whereas in other areas the expression of either SM22 or a-SMA was predominant.Twenty two out of 32 patients with MN showed stable renal function. TG2 immunostaining was increased in sections from patients with MN compared to healthy controls. TG2 at diagnosis was more intense in patients with more severe interstitial fibrosis and advanced glomerular sclerosis. TG2 significantly increased in most patients in the repeat biopsies whereas patients that showed a marked increase in interstitial fibrosis in the repeat biopsy had significantly more TG2 expression in the first biopsy.In conclusion, intense SM22 expression was observed in the renal tissue of patients with different types of GN. The co-localization study of SM22 and a–SMA suggests that different subpopulations of myofibroblasts might be involved in the development of kidney biopsy had significantly more TG2 expression in the first biopsy.In conclusion, intense SM22 expression was observed in the renal tissue of patients with different types of GN. The co-localization study of SM22 and a–SMA suggests that different subpopulations of myofibroblasts might be involved in the development of kidneyΗ παρουσία λευκωματουρίας αποτελεί δυσμενή προγνωστικό παράγοντα για τους ασθενείς με σπειραματονεφρίτιδα (ΣΝ) χωρίς εντούτοις αυτό να επιβεβαιώνεται πάντα. Συνεπώς, είναι επιβεβλημένη η εύρεση περισσότερο ειδικών προγνωστικών δεικτών που να αντανακλούν τη διαδικασία επούλωσης της βλάβης ή εξέλιξής της σε ίνωση. Σκοπός, της παρούσας μελέτης ήταν η αναγνώριση πρώιμων δεικτών εξέλιξης της νεφρικής βλάβης σε ασθενείς με σημαντικού βαθμού λευκωματουρία.Ως τέτοιοι προγνωστικοί δείκτες μελετήθηκαν η έκφραση της τρανσγελίνης (SM22) και της τρανσγλουταμινάσης–2 (TG2). Η SM22 είναι μια πρωτεΐνη που εκφράζεται στα λεία μυϊκά κύτταρα και αποτελεί δείκτη της επιθήλιο-μεσεγχυματικής μετάπτωσης. Η TG2 αποτελεί ένα ένζυμο που επάγει τη νεφρική ίνωση μεταβάλλοντας την ομοιόσταση της εξωκυτταρίου θεμέλιας ουσίας.Η έκφραση της SM22 μελετήθηκε με τη μέθοδο της ανοσοϊστοχημείας και του ανοσοφθορισμού, σε νεφρικές βιοψίες 67 ασθενών με διάφορους τύπους ΣΝ, και συσχετίστηκε με την κλινική τους πορεία μετά πάροδο πενταετούς παρακολούθησης. Επιπλέον, εξετάστηκε με τη μέθοδο του συνεντοπισμού, κατά πόσον η έκφραση της SM22 συμπίπτει με αυτήν της α–ακτίνης των λείων μυϊκών ινών (α–SMA). Η έκφραση της TG–2 μελετήθηκε με ανοσοφθορισμό σε νεφρικές βιοψίες από 32 ασθενείς με μεμβρανώδη νεφροπάθεια (ΜΝ). Όλοι οι ασθενείς με ΜΝ έλαβαν αγωγή με κορτικοειδή και κυκλοσπορίνη για 24 μήνες και σε 14 από αυτούς διενεργήθηκε επαναληπτική βιοψία και έγινε περαιτέρω μελέτη της TG2. Ως ομάδα ελέγχου για την έκφραση των παραπάνω μορίων χρησιμοποιήθηκαν τομές από υγιείς περιοχές νεφρών.Από τους 67 ασθενείς που μελετήθηκε η έκφραση της SM22, οι 46 διατήρησαν σταθερή νεφρική λειτουργία. Στις βιοψίες ελέγχου η έκφραση της SM22 περιορίστηκε στο τοίχωμα των αγγείων ενώ στους ασθενείς με ΣΝ επεκτάθηκε εντός των σπειραμάτων και του διάμεσου χώρου. Η SM22 βρέθηκε να σχετίζεται με το βαθμό σπειραματικής σκλήρυνσης και ίνωσης του διάμεσου χώρου, με το βαθμό μεσαγγειακής υπερπλασίας και την έκβαση της νεφρικής λειτουργίας. Η μελέτη συνεντοπισμού της SM22 και της α-SMA ανέδειξε περιοχές όπου οι δύο πρωτεΐνες εκφράζονταν ταυτόχρονα ενώ σε άλλες κάθε πρωτεΐνη εκφραζόταν χωριστά.Κατά το διάστημα παρακολούθησης οι 22 από τους 32 ασθενείς με ΜΝ παρουσίασαν σταθερή νεφρική λειτουργία. Η έκφραση της TG2 βρέθηκε αυξημένη στις βιοψίες των ασθενών με ΜΝ σε σχέση με την ομάδα ελέγχου. Η έκφραση της TG2 στις βιοψίες διάγνωσης ήταν περισσότερο αυξημένη στους ασθενείς με πιο έντονη διάμεση ίνωση και σπειραματική σκλήρυνση. Τέλος, η TG2 βρέθηκε αυξημένη στους περισσότερους ασθενείς στην επαναληπτική βιοψία, ενώ οι ασθενείς που παρουσίαζαν έντονη αύξηση της διάμεσης ίνωσης στην επαναληπτική βιοψία είχαν και εντονότερη έκφραση της TG2 κατά τη διάγνωση της νόσου.Συμπερασματικά, η έκφραση της SM22 βρέθηκε αυξημένη στο νεφρικό ιστό ασθενών με ΣΝ, ενώ η μελέτη συνεντοπισμού της SM22 και της α–SMA ανέδειξε την παρουσία πιθανώς διαφορετικών υποπληθυσμών μυοϊνοβλαστών. Όσον αφορά την TG2, η έντονη έκφραση της στο νεφρικό ιστό ασθενών με ΜΝ, η οποία καθίσταται εντονότερη μετά τη χορήγηση ανοσοκατασταλτικής αγωγής, υποδηλώνει τη συμμετοχή της TG2 στους μηχανισμούς βλάβης και εξέλιξης της ΜΝ. Επιπρόσθετα, η πρώιμη ανίχνευση της TG2 πιθανόν να έχει ιδιαίτερη σημασία στη ΜΝ καθώς η αυξημένη έκφρασή της φαίνεται να προηγείται της διάμεσης ίνωσης

Rhabdomyolysis and acute kidney injury after acupuncture sessions

Rhabdomyolysis is usually caused by muscle injury, drugs or alcohol and presents with muscle weakness and pain. It is characterized by rise in serum creatine kinase, aminotransferases and electrolytes as well as myoglobinuria. Myoglobinuria may cause acute kidney injury by direct proximal tubule cytotoxicity, renal vasoconstriction, intraluminal cast formation and distal tubule obstruction. Muscle pain and weakness as well as vascular injury have been reported after acupuncture. We report a case of severe rhabdomyolysis and acute kidney injury after acupuncture sessions

Membranoproliferative glomerulonephritis in a patient with chronic brucellosis

Brucellosis is the most common zoonotic disease in Greece, with an endemic distribution and can affect any organ. Infiltration of the renal parenchyma causes acute and chronic interstitial nephritis with granulomas, whereas renal glomeruli are rarely affected. The disease has been sporadically reported, and it causes various histopathologic patterns. Herein, we describe the case of a 39-year-old stock breeder with a history of recurrent episodes of bacteremia caused by Brucella melitensis over a period of 3 years. Two months after the last episode of bacteremia, he presented with mild renal insufficiency, nephrotic range proteinuria, and microscopic hematuria. A renal biopsy revealed membranoproliferative glomerulonephritis with a pattern of focal-segmental nodular sclerosis and moderate tubulointerstitial fibrosis. The patient received antimicrobial and corticosteroid therapy with partial remission of the nephrotic syndrome

Novel oxidized LDL-based clinical markers in peritoneal dialysis patients for atherosclerosis risk assessment

Maintenance peritoneal dialysis (PD) is commonly associated with cardiovascular diseases (CVDs), whose risk is assessed via LDL-C. Nonetheless, oxidized LDL (oxLDL), as being a key component of atherosclerotic lesions, could be also associated with atherosclerosis and related CVDs. However, its predictive value for CVDs risk assessment is subject of research studies due to the lack of specific methods to measure oxLDL status from its individual lipid/protein components. In the present study, six novel oxLDL markers, representative of certain oxidative modifications on the LDL protein and lipid components, are measured in atherosclerosis-prone PD patients (39) versus those in chronic kidney disease patients (61) under hemodialysis (HD) and healthy controls (40). LDL from serum of PD, HD and control subjects were isolated and fractionated into cholesteryl esters, triglycerides, free cholesterol, phospholipids and apolipoprotein B100 (apoB100). Subsequently the oxLDL markers cholesteryl ester hydroperoxides (-OOH), triglyceride-OOH, free cholesterol-OOH, phospholipid-OOH, apoB100 malondialdehyde and apoB100 dityrosines were measured. LDL carotenoid levels and LDL particle serum concentration were also measured. The levels of all oxLDL lipid-OOH markers were significantly elevated in PD patients versus control, while the levels of cholesteryl ester-/triglyceride-/free cholesterol-OOH were significantly elevated in PD versus HD patients, regardless of patients’ underlying medical conditions, sex, age, PD type, clinical biochemical markers and medication. It should be noted that all fractionated lipid-OOH levels were inversely correlated with LDL-P concentration, while LDL-P concentration was not correlated with LDL-C in PD patients. Moreover, LDL carotenoids were significantly lower in PD patients versus control. The increased levels of oxLDL status specific markers in both PD and HD patients (compared to control), support a potential prognostic value of oxLDL regarding CVD risk assessment in both patient groups. Lastly, the study introduces the oxLDL peroxidation markers free cholesterol-OOH and cholesteryl ester-OOH as complementary to LDL-P number, and as possible alternatives to LDL-C