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Introduction: Studies in cholesterol-fed rabbits showed that anti-proliferative chemotherapeutic agents such as paclitaxel associated with solid lipid nanoparticles (LDE) have marked anti-atherosclerotic effects. In addition, association with LDE nearly abolishes paclitaxel toxicity. We investigated whether treatment with LDE-paclitaxel changes plaque progression by coronary CT angiography and is safe in patients with chronic coronary artery disease. Methods: We conducted a prospective, randomized, double-blind, placebo-controlled pilot study in patients with multi-vessel chronic coronary artery disease. Patients were randomized to receive IV infusions of LDE-paclitaxel (paclitaxel dose: 175â mg/m2 body surface) or LDE alone (placebo group), administered every 3 weeks for 18 weeks. All participants received guideline-directed medical therapy. Clinical and laboratory safety evaluations were made at baseline and every 3 weeks until the end of the study. Analysis of inflammatory biomarkers and coronary CTA was also performed at baseline and 4 weeks after treatment. Results: Forty patients aged 65.6 ± 8 years, 20 in LDE-paclitaxel and 20 in placebo group were enrolled. Among those, 58% had diabetes, 50% had myocardial infarction, and 91% were in use of statin and aspirin. Baseline demographics, risk factors, and laboratory results were not different between groups. In all patients, no clinical or laboratory toxicities were observed. From the baseline to the end of follow-up, there was a non-significant trend toward a decrease in IL-6 levels and hsCRP in the LDE-paclitaxel group (-16% and -28%, respectively), not observed in placebo. Regarding plaque progression analysis, variation in plaque parameter values was wide, and no difference between groups was observed. Conclusion: In patients with multivessel chronic coronary artery disease and optimized medical therapy, LDE-paclitaxel was safe and showed clues of potential benefits in reducing inflammatory biomarkers. Clinical Trial Registration: https://clinicaltrials.gov/study/NCT04148833, identifier (NCT04148833).
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OBJECTIVE: Previously, lipid nanoparticles (LDE) injected in women with endometriosis were shown to concentrate in the lesions. Here, the safety and feasibility of LDE carrying methotrexate (MTX) to treat deep infiltrating endometriosis was tested. DESIGN: Prospective pilot study. SETTING: Perola Byington Hospital Reference for Women's Health. SUBJECTS: Eleven volunteers (aged 30-47 years, BMI 26.15 ± 6.50 kg/m2) with endometriosis with visual analog scale pelvic pain scores (VAS) > 7 and rectosigmoid lesions were enrolled in the study. INTERVENTION: Three patients were treated with LDE-MTX at single intravenous 25 mg/m2 dose of MTX and eight patients with two 25 mg/m2 doses with 1-week interval. MAIN OUTCOME MEASURES: Clinical complaints, blood count, and biochemistry were analyzed before treatment and on days 90, 120, and 180 after LDE-MTX administration. Endometriotic lesions were evaluated by pelvic and transvaginal ultrasound (TVUS) before treatment and on days 30 and 180 after LDE-MTX administration. RESULTS: No clinical complaints related with LDE-MTX treatment were reported by the patients, and no hematologic, renal, or hepatic toxicities were observed in the laboratorial exams. FSH, LH, TSH, free T4, anti-Müllerian hormone, and prolactin levels were also within normal ranges during the observation period. Scores for deep dyspareunia (p < 0.001), chronic pelvic pain (p = 0.008), and dyschezia (p = 0.025) were improved over the 180-day observation period. There was a non-significant trend for reduction of VAS scores for dysmenorrhea. Bowel lesions by TVUS were unchanged. No clear differences between the two dose levels in therapeutic responses were observed. CONCLUSION: Results support the safety and feasibility of using LDE-MTX in women with deep infiltrating endometriosis as a novel and promising therapy for the disease. More prolonged treatment schemes should be tested in future placebo-controlled studies aiming to establish the usefulness of this novel nanomedicine approach.
Subject(s)
Dyspareunia , Endometriosis , Liposomes , Nanoparticles , Humans , Female , Endometriosis/complications , Endometriosis/drug therapy , Endometriosis/pathology , Methotrexate/therapeutic use , Pilot Projects , Prospective Studies , Pelvic Pain/drug therapy , Pelvic Pain/etiology , Dysmenorrhea , Dyspareunia/drug therapy , Dyspareunia/etiologyABSTRACT
INTRODUCTION: HDL function has gained prominence in the literature as there is a greater predictive capacity for risk in early coronary artery disease when compared to the traditional parameters. However, it is unclear how dietary energy restriction and atorvastatin influence HDL function. METHODS: A randomized controlled trial with 39 women with early CAD divided into three groups (n = 13): energy restriction (30% of VET), atorvastatin (80 mg), and control. Analyses of traditional biochemical markers (lipid and glucose profile), circulating Sirt-1, and HDL function (lipid composition, lipid transfer, and antioxidant capacity). RESULTS: Participants' mean age was 50.5 ± 3.8 years. Energy restriction increased Sirt-1 by 63.6 pg/mL (95%CI: 1.5-125.7; p = 0.045) and reduced BMI by 0.8 kg/m2 (95%CI: -1.349--0.273; p = 0.004) in a manner independent of other cardiometabolic factors. Atorvastatin reduced LDL-c by 40.0 mg/dL (95%CI: -69.910--10.1; p = 0.010). Increased Sirt-1 and reduced BMI were independently associated with reduced phospholipid composition of HDL (respectively, ß = -0.071; CI95%:-0.136--0.006; p = 0.033; ß = 7.486; CI95%:0.350-14.622; p = 0.040). Reduction in BMI was associated with lower HDL-free cholesterol (ß = 0.818; CI95%:0.044-1.593; p = 0.039). LDL-c reduction by statins was associated with reduced maximal lipid peroxide production rate of HDL (ß = 0.002; CI95%:0.000-0.003; p = 0.022) and total conjugated diene generation (ß = 0.001; CI95%:0.000-0.001; p = 0.029). CONCLUSION: This study showed that energy restriction and atorvastatin administration were associated with changes in lipid profile, serum Sirt-1 concentrations, and HDL function.
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In Marfan syndrome (MFS), dilation, dissection, and rupture of the aorta occur. Inflammation can be involved in the pathogenicity of aortic defects and can thus be a therapeutic target for MFS. Previously, we showed that the formulation of methotrexate (MTX) associated with lipid nanoparticles (LDE) has potent anti-inflammatory effects without toxicity. To investigate whether LDEMTX treatment can prevent the development of aortic lesions in the MFS murine model. MgΔloxPneo MFS (n = 40) and wild-type (WT, n = 60) mice were allocated to 6 groups weekly injected with IP solutions of: (1) only LDE; (2) commercial MTX; (3) LDEMTX (dose = 1mg/kg) between 3rd and 6th months of life. After 12 weeks of treatments, animals were examined by echocardiography and euthanatized for morphometric and molecular studies. MFS mice treated with LDEMTX showed narrower lumens in the aortic arch, as well as in the ascending and descending aorta. LDEMTX reduced fibrosis and the number of dissections in MFS but not the number of elastic fiber disruptions. In MFS mice, LDEMTX treatment lowered protein expression of pro-inflammatory factors macrophages (CD68), T-lymphocytes (CD3), tumor necrosis factor-α (TNF-α), apoptotic factor cleaved-caspase 3, and type 1 collagen and lowered the protein expression of the transforming growth factor-ß (TGF-ß), extracellular signal-regulated kinases ½ (ERK1/2), and SMAD3. Protein expression of CD68 and CD3 had a positive correlation with an area of aortic lumen (r 2 = 0.36; p < 0.001), suggesting the importance of inflammation in the causative mechanisms of aortic dilation. Enhanced adenosine availability by LDEMTX was suggested by higher aortic expression of an anti-adenosine A2a receptor (A2a) and lower adenosine deaminase expression. Commercial MTX had negligible effects. LDEMTX prevented the development of MFS-associated aortic defects and can thus be a candidate for testing in clinical studies.
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INTRODUCTION: Low high-density lipoprotein (HDL)-cholesterol is frequent in patients with peripheral artery disease (PAD) and also in type 2 diabetes mellitus (T2DM), the major risk factor for PAD. The transfer of cholesterol from the other lipoproteins to HDL is an important aspect of HDL metabolism and function, and may contribute to atherogenic mechanisms that lead to PAD development. OBJECTIVE: The aim of this study was to investigate the status of cholesterol transfers in patients with PAD without or with T2DM. METHODS: Patients with PAD (n = 19), with PAD and T2DM (PAD + DM, n = 19), and healthy controls (n = 20), all paired for age, sex, and BMI were studied. Transfer of both forms of cholesterol, unesterified (UC) and esterified (EC), was performed by incubating plasma with a donor nanoemulsion containing radioactive UC and EC, followed by chemical precipitation and HDL radioactive counting. RESULTS: Low-density lipoprotein (LDL)-cholesterol and triglycerides were similar in the three groups. Compared to controls, HDL-C was lower in PAD + DM (p < 0.05), but not in PAD. Transfer of UC was lower in PAD + DM than in PAD and controls (4.18 ± 1.17%, 5.13 ± 1.44%, 6.59 ± 1.25%, respectively, p < 0.001). EC transfer tended to be lower in PAD + DM than in controls (2.96 ± 0.60 vs 4.12 ± 0.89%, p = 0.05). Concentrations of cholesteryl ester transfer protein (CETP) and lecithin-cholesterol acyltransferase (LCAT), both involved in HDL metabolism, were not different among the three groups. CONCLUSION: Deficient cholesterol transfer to HDL may play a role in PAD pathogenesis. Since UC transfer to HDL was lower in PAD + DM compared to PAD alone, it is possible that defective HDL metabolism may contribute to the higher PAD incidence in patients with T2DM.Keywords.
Subject(s)
Diabetes Mellitus, Type 2 , Peripheral Arterial Disease , Cholesterol , Cholesterol, HDL , Diabetes Mellitus, Type 2/diagnosis , Humans , Lipoproteins, HDL , Peripheral Arterial Disease/diagnosis , Peripheral Arterial Disease/epidemiologyABSTRACT
Introdução: A doença arterial coronária (DAC) decorrente da aterosclerose é uma das principais causas de comprometimento do envelhecimento saudável e sobrevida do idoso.Entre os principais fatores de risco da DAC estão o diabetes mellitus tipo 2 (DM) e as dislipidemias. O HDL-colesterol baixo é fator de risco importante, mas aspectos funcionais e metabólicos da HDL devem ser avaliados, já que esta lipoproteína tem várias ações anti-aterogênicas. Neste sentido, a transferência de lípides de outras lipoproteínas para a HDL, mediada pela proteína de transferência de ésteres de colesterol (CETP), é passo importante na formação e metabolismo da HDL e está relacionada com a presença de DAC. Objetivo: Avaliar o impacto da idade nas transferências de lípides para HDL e outros parâmetros relacionados com o metabolismo da HDL em indivíduos idosos e as mudanças nesses parâmetros em idosos com DAC e com DAC e DM. Métodos: Foram estudados 25 jovens (JOV), 35 idosos sem DAC e sem DM (IDS), 35 idosos com DAC (IDS-DAC) e 34 idosos com DAC e DM (IDS-DAC-DM). Foram determinados perfil lipídico e apolipoproteínas plasmáticas, concentração plasmática da CETP e da lecitina-colesterol aciltransferase (LCAT), composição lipídica e diâmetro da HDL e marcadores inflamatórios. A transferência de colesterol esterificado e livre, fosfolípides e triglicérides para a HDL foi realizada por ensaio "in vitro" com uma nanopartícula marcada com lípides radioativos como partícula doadora de lípides. Após a precipitação química das outras lipoproteínas e da nanopartícula doadora, o sobrenadante contendo HDL foi separadoe medida a radioatividade. Resultados: IDS apresentou IMC maior que JOV. LDL-colesterol e não-HDL-colesterol, IL-6 e IL-8 foram mais altos, IL-1ß mais baixo e a transferência de fosfolípides para a HDL foi maior em IDS do que em JOV, mas as diferenças desapareceram quando corrigidas pelo IMC. Entre IDS-DAC e IDS não houve diferenças nos lípides plasmáticos, mas no IDS-DAC a transferência de colesterol livre, triglicérides e fosfolípides foi menor e a de colesterol esterificado foi maior. A concentração de CETP foi maior no IDS-DAC, onde houve maior % de colesterol esterificado e triglicérides e menor % de fosfolípides na HDL. Em IDS-DAC-DM, apoB foi maior que em IDS-DAC, mas LDL-colesterol foi igual. Houve menor transferência de colesterol esterificado em IDS-DAC-DM comparado a IDS-DAC e maior de fosfolípides. IDS-DAC-DM teve CETP mais baixa e LCAT mais alta do que IDS-DAC. Em IDS-DAC-DM houve menor proporção de colesterol esterificado e livre e maior de fosfolípides na HDL. Marcadores inflamatórios não diferiram entre IDS-DAC-DM e IDS-DAC. Conclusões: As alterações nos parâmetros de transferência de lípides sinalizaram tanto a presença de DAC nos idosos quanto diferenciaram idosos com DAC associada a DM daqueles apenas com DAC. A redução da transferência de colesterol livre nos idosos com DAC é aterogênica, como foi mostrado em trabalho anteriorem indivíduos de 40-50 anos com DAC precoce. Esses dados podem ter aplicação tanto na prevenção quanto na terapêutica da DAC, por meio de medicamentos que modulem a transferência de lípides para a HDL e assim melhorem a função anti-aterogênica desta lipoproteína
Introduction: Coronary artery disease (CAD) resulting from atherosclerosis is one of the main causes of compromised healthy aging and lifespan in elderly people. Amongst the main risk factors for CAD are type 2 diabetes mellitus (DM) and dyslipidemias. Low HDL-cholesterol is an important risk factor, but functional and metabolic aspects of HDL must be evaluated, since this lipoprotein has several anti-atherogenic actions. In this regard, lipid transfer from other lipoproteins to HDL, mediated by cholesteryl ester transfer protein (CETP), is an important step towards the formation and metabolism of HDL and is related to the presence of CAD. Objective: To evaluate the impact of age in lipid transfer to HDL and other parameters related to HDL metabolism in elderly individuals and the changes in these parameters in elderly individuals with CAD and with CAD and DM. Methods: 25 young (YOUNG), 35 elderly without CAD and DM (ELDERLY), 35 elderly with CAD (ELDERLY-CAD) and 34 elderly with CAD and DM (ELDERLY-CAD-DM) subjects were studied. The lipid profile, the apolipoprotein, CETP and lecithin-cholesterol acyltransferase (LCAT) plasma concentration,theHDL lipid composition and diameter and inflammatory markers were evaluated.The transfer of esterified and free cholesterol, phospholipids and triglycerides to HDL was assayed in vitro with a donor lipid nanoparticle labeled with radioactive lipids.After chemical precipitation of the other lipoproteins and the donor lipid nanoparticle, the supernatant containing HDL was separated and the radioactivity was measured. Results: ELDERLY presented greater BMI than YOUNG. LDL-cholesterol and non-HDL-cholesterol, IL-6 and IL-8 were higher, IL-1ß was lower and phospholipid transfer to HDL was higher in ELDERLY than in YOUNG, but the differences disappeared when corrected by BMI. There were no differences in plasmatic lipids between ELDERLY-CAD and ELDERLY, but in ELDERLY-CAD the transfer of free cholesterol, triglycerides and phospholipids was lower and of esterified cholesterol was higher. CETP concentration was higher in ELDERLY-CAD, where there was higher % of esterified cholesterol and triglycerides and lower % of phospholipids in HDL. In ELDERLY-CAD-DM, apo B was higher than in ELDERLY-CAD, but LDL-cholesterol was equal. There was lower transfer of esterified cholesterol in ELDERLY-CAD-DM compared to ELDERLY-CAD and higher transfer of phospholipids. ELDERLY-CAD-DM had lower CETP and higher LCAT than ELDERLY-CAD. In ELDERLY-CAD-DM there was a smaller proportion of esterified and free cholesterol and greater proportion of phospholipids in HDL. Inflammatory markers did not differ between ELDERLY-CAD-DM and ELDERLY-CAD. Conclusions: The alterations in the parameters of lipid transfer not only signalled the presence of CAD in the elderly but also differentiated the elderly with CAD and DM from those with CAD only. The reduction of free cholesterol transfer in the elderly with CAD is atherogenic, as shown in a previous work on individuals of 40-50 years of agewith precocious CAD. This data may be applied both to the prevention and the therapeutics of CAD, by means of medicines that modulate lipid transfer to HDL and thus improve the anti-atherogenic function of this lipoprotein
Subject(s)
Humans , Animals , Male , Female , Pregnancy , Infant, Newborn , Infant , Child, Preschool , Child , Adolescent , Adult , Middle Aged , Aged , Coronary Disease/complications , Diabetes Mellitus, Type 2/complications , Lipoproteins, HDL/analysis , Metabolism , Survival Analysis , Lipids/pharmacologyABSTRACT
Plasma lipids have been extensively studied in sedentary and in subjects practicing exercise training, but not in extreme inactivity as occurs in bedridden patients. This is important for the care of bedridden patients and understanding the overall plasma lipid regulation. Here, we investigated plasma lipids, lipid transfers to HDL and inflammatory markers in bedridden patients. Fasting blood samples were collected from 23 clinically stable bedridden patients under long-term care (>90 days) and 26 normolipidemic sedentary subjects, paired for age and gender. In vitro transfer of four lipids to HDL was performed by incubating plasma with donor nanoparticles containing radioactive lipids. Total (193 ± 36 vs 160 ± 43, p = 0.005), LDL (124 ± 3 vs 96 ± 33 p = 0.003) and HDL-cholesterol (45 ± 10 vs 36 ± 13, p = 0.008), apolipoprotein A-I (134 ± 20 vs 111 ± 24, p = 0.001) and oxidized LDL (53 ± 13 vs 43 ± 12, p = 0.011) were lower in bedridden patients, whereas triglycerides, apolipoprotein B, CETP and LCAT were equal in both groups. Transfers of all lipids, namely unesterified cholesterol, cholesterol esters, triglycerides and phospholipids, to HDL were lower in bedridden patients, probably due to their lower HDL-cholesterol levels. Concentrations of IL-1ß, IL-6, IL-8, HGF and NGF were higher in bedridden patients compared to sedentary subjects. In conclusion, inactivity had great impact on HDL, by lowering HDL-cholesterol, apolipoprotein A-I and thereby cholesterol transfers to the lipoprotein, which suggests that inactivity may deteriorate HDL protection beyond the ordinary sedentary condition.
Subject(s)
Apolipoprotein A-I/analysis , Biomarkers/blood , Cholesterol, HDL/blood , Inflammation/metabolism , Lipoproteins, LDL/analysis , Adult , Apolipoprotein A-I/blood , Bedridden Persons , Cholesterol Esters , Female , Hepatocyte Growth Factor/blood , Humans , Interleukin-6/blood , Interleukin-8/blood , Lipids/blood , Lipoproteins, LDL/blood , Male , Middle Aged , Nerve Growth Factor/blood , Sedentary BehaviorABSTRACT
It is well established that the development of insulin resistance shows a temporal sequence in different organs and tissues. Moreover, considering that the main aspect of insulin resistance in liver is a process of glucose overproduction from gluconeogenesis, we investigated if this metabolic change also shows temporal sequence. For this purpose, a well-established experimental model of insulin resistance induced by high-fat diet (HFD) was used. The mice received HFD (HFD group) or standard diet (COG group) for 1, 7, 14 or 56 days. The HFD group showed increased (P < 0.05 versus COG) epididymal, retroperitoneal and inguinal fat weight from days 1 to 56. In agreement with these results, the HFD group also showed higher body weight (P < 0.05 versus COG) from days 7 to 56. Moreover, the changes induced by HFD on liver gluconeogenesis were progressive because the increment (P < 0.05 versus COG) in glucose production from l-lactate, glycerol, l-alanine and l-glutamine occurred 7, 14, 56 and 56 days after the introduction of the HFD schedule, respectively. Furthermore, glycaemia and cholesterolemia increased (P < 0.05 versus COG) 14 days after starting the HFD schedule. Taken together, the results suggest that the intensification of liver gluconeogenesis induced by an HFD is not a synchronous 'all-or-nothing process' but is specific for each gluconeogenic substrate and is integrated in a temporal manner with the progressive augmentation of fasting glycaemia.
Subject(s)
Diet, High-Fat , Glucose/metabolism , Liver/metabolism , Animals , Blood Glucose/analysis , Body Weight , Cholesterol/blood , Gluconeogenesis , Insulin Resistance , Male , Mice , Time Factors , Triglycerides/bloodABSTRACT
We previously demonstrated an increased liver gluconeogenesis (LG) during insulin-induced hypoglycaemia. Thus, an expected effect of sulphonylureas induced hypoglycaemia (SIH) could be the activation of LG. However, sulphonylureas infused directly in to the liver inhibits LG. Considering these opposite effects we investigated herein LG in rats submitted to SIH. For this purpose, 24 h fasted rats that received glibenclamide (10 mg kg(-1) ) were used (SIH group). Control group received oral saline. Glycaemia at 30, 60, 90, 120 and 150 min after oral administration of glibenclamide were evaluated. Since the lowest glycaemia was obtained 120 min after glibenclamide administration, this time was chosen to investigate LG in situ perfused livers. The gluconeogenesis from precursors that enters in this metabolic pathway before the mitochondrial step, i.e. L-alanine (5 mM), L-lactate (2 mM), pyruvate (5 mM) and L-glutamine were decreased (p < 0·05). However, the gluconeogenic activity using glycerol (2 mM), which enters in the gluconeogenesis after the mitochondrial step was maintained. Taken together, the results suggest that the inhibition of LG promoted by SIH overcome the activation of this metabolic pathway promoted by IIH and could be attributed, at least in part, to its effect on mitochondrial function.
