Low-dose spironolactone-pioglitazone-metformin normalizes circulating fetuin-a concentrations in adolescent girls with polycystic ovary syndrome

BACKGROUND: Fetuin-A is a glycoprotein produced in the liver and related to metabolic syndrome; fetuin-A secretion is divergently regulated in different pathological conditions. In girls with polycystic ovary syndrome (PCOS), insulin sensitization results in a more favorable endocrine-metabolic outcome than oral contraception; we assessed whether those differences are underscored by changes in circulating fetuin-A. METHODS: Fetuin-A concentration endocrine-metabolic markers and hepatovisceral fat were measured longitudinally in 35 PCOS girls [age, 16 yr; body mass index (BMI), 23 kg/m2] randomized to receive either oral contraception [ethinylestradiol-levonorgestrel (n = 18)] or a low-dose combination of spironolactone, pioglitazone, and metformin (SPIOMET, n = 17) over 12 months. Healthy adolescent girls (age- and BMI-matched) were used as controls (n = 25). RESULTS: Pretreatment fetuin-A serum levels in PCOS girls were lower than those in controls. After 12 months on treatment, fetuin-A raised to control levels only in the SPIOMET subgroup (P = 0.009, versus oral contraception); this increase was paralleled by a healthier metabolic profile with less hepatic fat (by MRI); baseline serum fetuin-A as well as the changes over 12 months was inversely related to hepatic adiposity. CONCLUSIONS: A low-dose combination of insulin sensitizers and an antiandrogen-but not oral contraception-normalizes fetuin-A levels in adolescent girls with PCOS. This trial is registered with ISRCTN29234515

Adipose tissue aging partially accounts for fat alterations in HIV lipodystrophy

Altres ajuts: European Regional Development Fund (FEDER).Lipodystrophy is a major disturbance in people living with HIV-1 (PLWH). Several systemic alterations in PLWH are reminiscent of those that occur in ageing. It is unknown whether the lipodystrophy in PLWH is the consequence of accelerated ageing in adipose tissue. We compared systemic and adipose tissue disturbances in PLWH with those in healthy elderly individuals (~80 y old). We observed similarly enhanced expression of inflammation-related genes and decreased autophagy in adipose tissues from elderly individuals and PLWH. Indications of repressed adipogenesis and mitochondrial dysfunction were found specifically in PLWH, whereas reduced telomere length and signs of senesce were specific to elderly individuals. We conclude that ageing of adipose tissue accounts only partially for the alterations in adipose tissues of PLWH

Effects of Switching from Stavudine to Raltegravir on Subcutaneous Adipose Tissue in HIV-Infected Patients with HIV/HAART-Associated Lipodystrophy Syndrome (HALS). A Clinical and Molecular Study

HIV-1/HAART-associated lipodystrophy syndrome (HALS) has been associated with exposure to stavudine (d4T) through mitochondrial dysfunction. We performed a 48-week study to assess the effects of switching from d4T to raltegravir (RAL) on metabolic and fat molecular parameters of patients with HALS. Forty-two patients with HALS and a median exposure to d4T > 7 years were switched to RAL and followed for 48 weeks. Fasting metabolic tests, HIV RNA, CD4 cell count, and fat measured by DEXA were obtained at baseline and week 48. mtDNA and gene transcripts for PPAR gamma, adiponectin, cytochrome b, Cox IV, TNF alpha, MCP-1 and CD68 were assessed in paired subcutaneous fat tissue biopsies. Lipid parameters, fasting glucose, insulin, and HOMA-IR did not change significantly. Whole body fat (P = 0.0027) and limb fat mass (P<0.0001) increased from baseline. Trunk/limb fat ratio (P = 0.0022), fat mass ratio (P = 0.0020), fat mass index (P = 0.0011) and percent leg fat normalized to BMI (P<0.0001) improved after 48 weeks. Relative abundance of mtDNA, expression of PPAR gamma, adiponectin, Cyt b, and MCP-1 genes increased, whereas Cox IV, TNF alpha, and CD68 did not change significantly from baseline. Switching from d4T to RAL in patients with HALS is associated with an increase in limb fat mass and an improvement in markers of adipocyte differentiation and mitochondrial function in SAT

The molecular signature of HIV-1-associated Lipomatosis reveals differential involvement of Brown and Beige/Brite Adipocyte cell lineages

Highly active antiretroviral therapy has remarkably improved quality of life of HIV-1-infected patients. However, this treatment has been associated with the so-called lipodystrophic syndrome, which conveys a number of adverse metabolic effects and morphological alterations. Among them, lipoatrophy of subcutaneous fat in certain anatomical areas and hypertrophy of visceral depots are the most common. Less frequently, lipomatous enlargements of subcutaneous fat at distinct anatomic areas occur. Lipomatous adipose tissue in the dorso-cervical area ('buffalo hump') has been associated with a partial white-to-brown phenotype transition and with increased cell proliferation, but, to date, lipomatous enlargements arising in other parts of the body have not been characterized. In order to establish the main molecular events associated with the appearance of lipomatosis in HIV-1 patients, we analyzed biopsies of lipomatous tissue from 'buffalo hump' and from other anatomical areas in patients, in comparison with healthy subcutaneous adipose tissue, using a marker gene expression approach. Both buffalo-hump and non-buffalo-hump lipomatous adipose tissues exhibited similar patterns of non-compromised adipogenesis, unaltered inflammation, non-fibrotic phenotype and proliferative activity. Shorter telomere length, prelamin A accumulation and SA-β-Gal induction, reminiscent of adipocyte senescence, were also common to both types of lipomatous tissues. Buffalo hump biopsies showed expression of marker genes of brown adipose tissue (e.g. UCP1) and, specifically, of 'classical' brown adipocytes (e.g. ZIC1) but not of beige/brite adipocytes. No such brown fat-related gene expression occurred in lipomatous tissues at other anatomical sites. In conclusion, buffalo hump and other subcutaneous adipose tissue enlargements from HIV-1-infected patients share a similar lipomatous character. However, a distorted induction of white-to-'classical brown adipocyte' phenotype appears unique of dorso-cervical lipomatosis. Thus, the insults caused by HIV-1 viral infection and/or antiretroviral therapy leading to lipomatosis are acting in a location- and adipocyte lineage-dependent manner

Bases moleculares de las alteraciones del tejido adiposo y cambios metabólicos asociados al síndrome lipodistrófico en pacientes infectados por HIV-1

El uso de la terapia HAART (Highly-Active-Antiretroviral-Therapy), puede dar lugar a múltiples efectos secundarios. El más frecuente de ellos es el denominado HALS (“HIV-infection, HAARTtreatment- associated-lipodystrophy-syndrome”) que comprende alteraciones como la lipoatrofia periferica; un aumento de tejido adiposo visceral o la lipomatosis del tejido adiposo. Además, estas alteraciones fisiológicas pueden ir acompañadas de alteraciones metabólicas. Para saber la aportación individual de algunos fármacos al desarrollo del síndrome lipodistrófico HALS se realizó un estudio de los efectos de Efavirenz, Nevirapina (NNRTIs) y Kaletra (PI) sobre adipocitos primarios de linaje blanco en cultivo. Efavirenz, que no era considerado un fármaco asociado al síndrome lipodistrófico, es capaz de inhibir la adipogénesis con mayor potencia que Kaletra y Nevirapina. Ninguno de estos fármacos provoca toxicidad mitocondrial por lo que sus efectos ocurren en ausencia de toxicidad mitocondrial. Tanto efavirenz como kaletra reducen la secreción de adipoquinas y aumentan la expresión y secreción de citoquinas relacionadas con la inflamación, pero estos efectos siempre son mayores con el EFV mientras la Nevirapina parece no afectar a este tipo de secreciónes. Para estudiar las características moleculares de los diferentes depósitos de tejido adiposo con comportamiento opuesto como el tejido adiposo subcutáneo lipoatrófico y el tejido adiposo visceral lipohipertrófico o el tejido adiposo lipomatoso de las “buffalo-hump” de los pacientes se han comparado características moleculares de ellas con tejido adiposo de individuos control. En la comparación entre el tejido adiposo subcutáneo lipoatrófico y el visceral se ha observado que en ambos casos el tejido adiposo presenta alteraciones similares en la función mitocondrial. En cambio el descenso de marcadores de adipogénesis observado en el tejido subcutáneo de pacientes no se reproduce en el tejido visceral. Este hecho, acompañado de diferencias en el perfil de expresión de marcadores de inflamación (que parece más leve en el tejido visceral), podría explicar el comportamiento opuesto de ambos depósitos en pacientes. El estudio en el que se compararon el tejido adiposo lipomatosos de las “buffalo-hump” y el tejido adiposo subcutáneo lipoatrófico de pacientes infectados por el HIV- indica que el tejido adiposo de las “buffalo-hump” presenta alteraciones especificas en la expresión génica respecto al tejido lipoatrófico en las que destaca una expresión normal de genes adipogénicos. Así mismo, el tejido lipomatoso es capaz de expresar UCP1, un gen característico del tejido adiposo marrón, y su capacidad proliferativa concuerda más con un fenotipo del tipo marrón, por lo que se puede decir que estos adipocitos tienen un fenotipo intermedio entre blanco y marrón que se mantiene cuando este tejido lipomatoso es utilizado para trasplante autólogo a la zona facial lipoatrófica en la que mantiene la proliferación desarrollándose el síndrome hámster. No se observan diferencias en las alteraciones mitocondriales observadas en ambos tejidos. Por otra parte la ausencia de un estado de inflamación local en BH podría explicar en parte este comportamiento diferente de ambos tejidos. Además se ha observado que los pacientes muestran niveles elevados de FGF21 y disminuidos de FGF19 (dos agentes homeostaticos) respecto a los controles. Estas diferencias con los controles se acentúan a medida que los pacientes infectados por el virus HIV-1 pasan de ser no tratados a tratados y aun más al desarrollar la lipodistrofia. Los niveles de FGF21 en suero se correlacionaban con indicadores de sensibilidad a insulina o marcadores de síndrome metabólico así como con marcadores de daño hepático que podrían estar relacionados con esteatosis hepática. Los niveles disminuidos en suero de FGF19 se correlacionan negativamente con parámetros indicativos de resistencia a insulina. Además se ha descrito en esta tesis que los receptores de estos agentes endocrinos FGFR1 y β-Klotho aparecen disminuidos en el tejido adiposo de los pacientes infectados por el virus HIV-1.Molecular basis of adipose tissue alterations and metabolic disturbances associated to HIV-1-infected lipodystrophic patients Disturbances in adipose tissue in HIV-1-infected patients undergoing HAART involve a complex set of alterations known as HAART-associated-lipodystrophy-syndrome (HALS). In most cases, lipoatrophy occur in the face, arms and legs. An enlargement of visceral adipose tissue, reminiscent of visceral obesity, is present often in combination with peripheral lipoatrophy. Lipomatosis is also commonly found in HALS, usually as an enlargement in the dorso-cervical area (buffalo-hump), although the development of lipomas in distinct anatomical sites has also been reported. This adipose tissue redistribution is associated with systemic metabolic alterations such as insulin resistance or dyslipidemia. To determine the individual contribution to HALS of some HAART-prescriptioned drugs, we performed an assessment of the effects of efavirenz, nevirapine and Kaletra on human cultured adipocytes. Our results support the fact that efavirenz and Kaletra impair adipogenesis, reduce the release of adipokines and increase the expression and release of inflammation-related cytokines, while nevirapine does not. Overall, those effects are greater in the case of efavirenz. We compared as well the molecular signature of subcutaneous lipoatrophic, visceral lipohipertrophic and dorso-cervical lipomatous adipose tissues from patients in order to determine the molecular basis causing these fat depots to behave in an opposite way. All fat biopsies from patients exhibited alterations in mitochondrial function marker genes. Visceral and “buffalo hump” fat didn’t show any alterations in the expression of adipogenesis marker genes when compared to healthy controls, while subcutaneous fat showed lower levels. The inflammatory profile was normal in “buffalo hump”, whereas visceral and subcutaneous adipose tissue depots exhibited a distinct, more exacerbated, pro-inflammatory profile. These differences could be part of the explanation of the mentioned different behavior. The serum levels of novel homeostatic agents FGF19 and FGF21 was also assessed in samples from lipodystrophic patients. FGF21 levels were significantly higher in patients and correlated positively with markers of insulin resistance, metabolic syndrome and hepatic damage. On the other hand, FGF19 levels were significantly lower in patients and correlated negatively with markers of insulin resistance. We studied the transcription level of FGF receptors in adipose tissue as well, resulting in a lower expression in biopsies from HALS patients

Modelling of knitted fabric deformation

Available from British Library Document Supply Centre-DSC:DXN050077 / BLDSC - British Library Document Supply CentreSIGLEGBUnited Kingdo

Nadir CD4 T cell count as predictor and high CD4 T cell intrinsic apoptosis as final mechanism of poor CD4 T cell recovery in virologically suppressed HIV-infected patients: clinical implications

BACKGROUND: Although antiretroviral therapy improves immune response, some human immunodeficiency virus-infected patients present unsatisfactory CD4 T cell recovery despite achieving viral suppression, resulting in increased morbidity and mortality. METHODS: Cross-sectional, case-control study to characterize the mechanism and to identify predictive factors of poor immune response. We included 230 patients who were receiving highly active antiretroviral therapy and who had a viral load 2 years; 95 were "discordant" (case patients; CD4 T cell count always <350 cells/microL), and 135 were "concordant" (control subjects). Activation markers, CD4 T cell death (necrosis, intrinsic apoptosis, and extrinsic apoptosis), and caspase-3 were measured. Clinical parameters, particularly antiretroviral combinations, were correlated with immune recovery. RESULTS: Discordant patients showed higher levels of activation markers, mainly in CD4 T cells (p < .001), and higher rates of spontaneous cell death (P < .001). Rates of activation and rates of CD4 T cell death (mainly by intrinsic apoptosis) were the best predictive factors for immune recovery, along with nadir CD4 T cell count. Patients who were receiving a protease inhibitor-based regimen were more likely to be discordant and showed higher rates of activation (P= .011), higher rates of CD4 T cell death (P = .033), and a lower nadir CD4 T cell count (P < .001). Multivariate analysis, however, ruled out any effect of protease inhibitors on immune recovery. No differences were observed between the use of tenofovir-emtricitabine (Truvada) and the use of abacavir-lamivudine (Kivexa). CONCLUSIONS: CD4 T cell apoptosis by the intrinsic pathway represents the determinant mechanism of the unsatisfactory immune recovery and should be targeted to manage therapy for discordant patients. The predictive value of low nadir CD4 T cell count for a poor immune recovery led us to consider starting antiretroviral therapy earlier. No differences were observed among antiretrovirals in terms of immune recovery

The Molecular Signature of HIV-1-Associated Lipomatosis Reveals Differential Involvement of Brown and Beige/Brite Adipocyte Cell Lineages.

Highly active antiretroviral therapy has remarkably improved quality of life of HIV-1-infected patients. However, this treatment has been associated with the so-called lipodystrophic syndrome, which conveys a number of adverse metabolic effects and morphological alterations. Among them, lipoatrophy of subcutaneous fat in certain anatomical areas and hypertrophy of visceral depots are the most common. Less frequently, lipomatous enlargements of subcutaneous fat at distinct anatomic areas occur. Lipomatous adipose tissue in the dorso-cervical area ("buffalo hump") has been associated with a partial white-to-brown phenotype transition and with increased cell proliferation, but, to date, lipomatous enlargements arising in other parts of the body have not been characterized. In order to establish the main molecular events associated with the appearance of lipomatosis in HIV-1 patients, we analyzed biopsies of lipomatous tissue from "buffalo hump" and from other anatomical areas in patients, in comparison with healthy subcutaneous adipose tissue, using a marker gene expression approach. Both buffalo-hump and non-buffalo-hump lipomatous adipose tissues exhibited similar patterns of non-compromised adipogenesis, unaltered inflammation, non-fibrotic phenotype and proliferative activity. Shorter telomere length, prelamin A accumulation and SA-β-Gal induction, reminiscent of adipocyte senescence, were also common to both types of lipomatous tissues. Buffalo hump biopsies showed expression of marker genes of brown adipose tissue (e.g. UCP1) and, specifically, of "classical" brown adipocytes (e.g. ZIC1) but not of beige/brite adipocytes. No such brown fat-related gene expression occurred in lipomatous tissues at other anatomical sites. In conclusion, buffalo hump and other subcutaneous adipose tissue enlargements from HIV-1-infected patients share a similar lipomatous character. However, a distorted induction of white-to-"classical brown adipocyte" phenotype appears unique of dorso-cervical lipomatosis. Thus, the insults caused by HIV-1 viral infection and/or antiretroviral therapy leading to lipomatosis are acting in a location- and adipocyte lineage-dependent manner