Efeito da inibição da produção de TNF-alfa por meio da administração de pentoxifilina na pancreatite aguda experimental / Effect of inhibition of TNF-alpha production by pentoxifylline administration in experimental acute pancreatitis

André Siqueira Matheus

20 September 2006

Pancreatite aguda é uma das principais causas de síndrome da resposta inflamatória sistêmica (SRIS). Complicações sistêmicas são os principais fatores responsáveis pela ocorrência de falência de múltiplos órgãos e sistemas e morte durante a primeira etapa da doença. Os níveis de mediadores inflamatórios possuem uma relação com a gravidade da pancreatite. O TNF-alfa tem sido descrito como o agente iniciador da resposta inflamatória da pancreatite aguda. Estudos prévios usando a pentoxifilina para bloquear a produção de TNF-alfa têm demonstrado efeitos benéficos quando usada em modelos experimentais de sepse ou choque. A infecção pancreática é a mais grave complicação da pancreatite aguda com índices de mortalidade que podem chegar a 80%. Os mecanismos que determinam a ocorrência da infecção pancreática não são bem esclarecidos. Objetivo: Determinar o efeito da inibição da produção de TNF-alfa na pancreatite aguda com a administração de pentoxifilina. Métodos: Foi utilizado um modelo experimental de pancreatite aguda grave através da injeção intraductal de taurocolato de sódio a 2,5%. Cento e vinte e quatro ratos Wistar machos foram divididos em três grupos: Controle (animais submetidos ao procedimento cirúrgico sem a administração de taurocolato de sódio), Pancreatite (animais submetidos à indução da pancreatite aguda) e Pentoxifilina (animais submetidos à indução da pancreatite aguda seguida da administração intraperitoneal de 25 mg/Kg de pentoxifilina). Foi realizada a dosagem sérica das interleucinas 6 e 10 e TNF-alfa duas horas após a indução da pancreatite. Foram analisadas a ocorrência de translocação bacteriana e a incidência de infecção pancreática, através de culturas realizadas 24 horas após a indução da pancreatite aguda e a mortalidade global. A ocorrência de infecção pancreática foi considerada como positiva quando a concentração de bactérias expressa em UFC/g foi maior que 105. Resultados: Quando comparado ao grupo Pancreatite, o grupo Pentoxifilina apresentou redução significativa da lesão histológica pancreática, dos níveis de IL-6, IL-10 e TNF-alfa e da ocorrência de infecção pancreática (p < 0,05), tais alterações se associam a redução significativa da mortalidade no grupo Pentoxifilina. Conclusão: A inibição da produção de TNF-alfa através da administração de pentoxifilina foi capaz de reduzir o processo inflamatório local e sistêmico, reduzir a translocação bacteriana e infecção pancreática e melhorar a sobrevida com redução dos índices de mortalidade desta grave doença / Acute pancreatitis (AP) is considered one of the typical conditions causing systemic inflammatory response (SIRS). Systemic complications are the most important contributors to multiple organ failure and death during the first stages of severe acute pancreatitis. Levels of pro-inflammatory cytokines increase during the course of AP, and these levels appear to be correlated with the severity of pancreatic inflammation. TNF-alfa may be an initiator of inflammatory process in AP. Previous studies using pentoxifylline to block TNF-alfa production have showed beneficial effects in experimental models of sepsis and shock. The gut is a target organ of the SIRS causing gut barrier dysfunction allowing bacteria and toxin translocation. Bacterial translocation has been implicated in the development of multiple organ failure and is one of the major causes of pancreatic infection in patients with pancreatic necrosis. Aim: To determinate the effects of inhibition of TNF-? on the pancreatic and systemic inflammatory response, pancreatic infection, and mortality rate in necrotizing acute pancreatitis in rats. Methods: An experimental model of severe AP by injection of 0.5ml of 2.5% sodium taurocholate into the pancreatic duct was utilized. A hundred and twenty four male Wistar rats were divided in 3 groups: Sham (surgical procedure without AP induction), Pancreatitis (AP Induction), and Pentoxifylline (AP induction plus administration of 25 mg/kg pentoxifylline). Pancreatic inflammatory response was measured by histological studies and systemic inflammatory response was analyzed measuring the production of inflammatory cytokines (IL-6, IL-10, and TNF-alfa). Pancreatic infection was evaluated with bacterial cultures performed 24 h after the AP induction. The numbers of organisms were expressed as colony forming units (CFU) per gram. The occurrence of pancreatic infection was also analyzed and considered positive when the CFU/g was > 105. A parallel survival study was also performed. Results: Inhibition of TNF-alfa by pentoxifylline shows beneficial effects in this experimental model. The Pentoxifylline group had a statistically significant reduction of histological damage in the pancreas, inflammatory cytokines levels (IL-6, IL-10, and TNF-?), and occurrence of pancreatic infection (p < 0.05). These changes were associated with a significant reduction of mortality rate. Conclusions: Inhibition of TNF-alfa reduced local and systemic inflammatory response, reduced systemic complication as pancreatic infection, and decrease mortality rate in this model. Pentoxifylline may provide a useful therapy in the treatment of acute pancreatitis

Ácido taurocólico

Fator de necrose tumoral

Interleucinas

Modelos animais

Pâncreas/microbiologia

Pancreatite necrosante aguda

Pentoxifilina/administração e dosagem

Ratos Wistar

Experimental model

Interleukins

Pancreas/microbiology

Pancreatitis acute necrotizing

Pentoxifylline/administration and dosage

Rats Wistar

Taurocholic acid

Tumor necrosis factor-alpha

Interaction between tin/flouride-containing solutions and artificially created dental pellicles on erosion prevetion in vitro

Algarni, Amnah Abdullah A.

January 2013

Indiana University-Purdue University Indianapolis (IUPUI)School of dentistry / BACKGROUND: Fluoride and stannous ions have been reported to be relevant for dental erosion prevention. However, their interaction with the acquired dental pellicle (ADP), a clinically relevant erosion protective factor, is not well known and needs to be investigated. OBJECTIVES: To investigate the anti-erosive properties of fluoride-containing solutions and stannous solutions on enamel and dentin surfaces with a previously formed ADP. To characterize the protein profile of the ADP treated with the test solutions. METHODS: Phase I tested four solutions: SnCl2/NaF, NaF, SnCl2 and deionized water (DIW) (as negative control). Forty bovine enamel and dentin specimens 104 (4x4x2 mm3) were prepared and randomly distributed into 4 groups (n = 10). The specimens were incubated in clarified human saliva (CHS) for 24 h for pellicle formation and then they were subjected to a cycling procedure that included a 5-min erosive challenge (0.3-percent citric acid, pH 2.6); a 2-min treatment with the solution (between 1st, 3rd and 6th cycles); a 2-h immersion in CHS, and overnight immersion in CHS. Cycles were repeated 6x/day for 5 days. The outcome measure was surface loss (SL) using profilometry. Phase II: Thirty-two (32) bovine enamel specimens (882 mm3) (n = 8) were similarly prepared and incubated in saliva for 24 h and then treated with the solutions for 2 min followed by CHS immersion for 2 h. This cycle was repeated 3x for one day. The pellicles formed and treated with the test rinse solutions were collected, digested, and analyzed for specific protein content using liquid chromatography electrospray ionization tandem mass spectrometry (LCESI-MS/MS). RESULTS: Phase I: for enamel, SnCl2/NaF, SnCl2, NaF solutions provided 89 percent, 67 percent, and 42 percent SL reduction respectively compared with the control, while in dentin they provided 60 percent, 23 percent, and 36 percent, respectively, all significant at p < 0.05. Phase II: Seventy-two (72) common proteins were identified in all groups, 30 exclusive to DIW, 20 to SnCl2/NaF, 19 to NaF, and 13 to SnCl2. SnCl2/NaF increased the abundance of pellicle proteins than each one alone. CONCLUSION: SnCl2/NaF showed the best anti-erosive effect on both enamel and dentin. The findings suggest that the composition of acquired pellicle changes with different solutions, which may be related to their anti-erosive effect.

Erosion

Enamel

Dentin

Proteins

Pellicle

Cariostatic Agents -- therapeutic use

Dental Pellicle -- physiology

Tooth Erosion -- prevention and control

Dental Enamel -- drug effects

Dental Enamel Solubility -- drug effects

Dentin -- drug effects

Septic Arthritis Associated With Chickenpox

Feierabend, R H.

01 November 1991

No description available.

adolescent

therapeutic use)

arthritis

infectious (diagnosis

drug therapy

etiology)

arthroscopy

chickenpox (complications)

child

preschool

drainage

female

humans

infant

knee

male

streptococcal infections (diagnosis

drug therapy

etiology)

streptococcus pyogenes

Family Medicine

Topical Absorption of Isopropyl Alcohol Induced Cardiac and Neurologic Deficits in an Adult Female With Intact Skin

Leeper, S C., Almatari, A L., Ingram, J D., Ferslew, K. E.

01 February 2000

Topical exposure to isopropyl alcohol has been reported in the literature to be toxic if sufficient isopropyl alcohol is absorbed (1-5). A clinical case is reported where a 48-y-old female presented with multiple unexplained cardiac and neurological deficits. The woman had developed the deficits over a 6-mo period in which she had been soaking towels with isopropyl alcohol and applying then to her skin overnight to ease arm pain she was experiencing. Cessation of the isopropyl alcohol exposure resolved her deficits within 3 d. A controlled repeat dermal exposure to isopropyl alcohol under clinical observation reproduced the deficits noted with corresponding serum and urine concentrations of isopropyl alcohol and acetone. Cessation of topical isopropyl alcohol exposure lead to subsequent resolution of all toxicities.

2-propanol (administration & dosage

adverse effects

pharmacokinetics)

administration

topical

female

heart (drug effects)

humans

middle aged

palliative care

therapy)

skin absorption

syncope (chemically induced)

Internal Medicine

Ultrasound-Guided Percutaneous Thrombin Injection for Femoral Artery Pseudoaneurysms

McCoy, Dana W., Scharfstein, B, Walker, W., Evans, J.

01 October 2000

We reviewed 13 cases of ultrasound-guided thrombin injection of femoral pseudoaneurysms. All cases occurred within a 17-month period from January 1998 through May 1999 and were complications of femoral artery puncture. Immediate total thrombosis occurred in nine of 13 patients. Twenty-four-hour follow-up ultrasound in seven patients revealed no recurrence of pseudoaneurysm. Two of 13 patients required operative repair. One pseudoaneurysm thrombosed with 15 minutes of compression after injection and one case required a second injection. No cases of arterial thrombosis were noted. Ultrasound-guided thrombin injection for femoral artery pseudoaneurysm represents a safe and effective alternative to operative repair.

aged

aged

80 and over

aneurysm

false (diagnostic imaging

drug therapy

etiology)

angioplasty

balloon

coronary

cardiac catheterization

female

femoral artery (diagnostic imaging)

humans

iatrogenic disease

injections

intralesional

male

middle aged

thrombin (administration & dosage)

treatment outcome

ultrasonography

doppler

color

Surgery

Improving the safety of chemotherapy administration: an oncology nurse-led failure mode and effects analysis

Ashley, L.J., Dexter, R., Marshall, F., McKenzie, B., Ryan, M., Armitage, Gerry R.

January 2011

No / PURPOSE/OBJECTIVES: To assess and improve the safety of hospital-based adult chemotherapy administration. DESIGN: Prospective, systems-focused clinical risk assessment. SETTING: An adult inpatient and outpatient oncology unit in a large urban hospital in the United Kingdom. SAMPLE: 8-person nurse-led multidisciplinary team, which included managerial staff and patient safety researchers. METHODS: Failure mode and effects analysis (FMEA), a prospective, systems-focused risk assessment methodology, was undertaken in biweekly team meetings and included mapping the chemotherapy administration process, identifying and numerically prioritizing potential errors (failure modes) for each process step, and generating remedial strategies to counteract them. MAIN RESEARCH VARIABLES: The analysis aimed to identify chemotherapy administration failure modes and to generate remedial strategies to address them. User feedback on the FMEA process also was collected. FINDINGS: Several specific chemotherapy failure modes were identified, the majority of which had not previously been recognized, and several novel strategies to counteract them were generated. Many of the strategies were specific, environment-focused actions, which are simple, quick, and inexpensive to implement; however, more substantive, longer-term initiatives also were generated. User feedback generally was very positive, and the process of undertaking the analysis improved multidisciplinary teamwork and communication. CONCLUSIONS: Although time and resource intensive, FMEA is a useful safety improvement tool. IMPLICATIONS FOR NURSING: Nurses should be aware of and informed about FMEA as a tool they can use in partnership with management and other disciplines to proactively and collectively improve the safety of high-risk oncology procedures such as chemotherapy administration.

Adult

Great Britain

Hospitals

Urban

Humans

Nursing Methodology Research

*Oncology Nursing

Prospective Studies

Risk Assessment/methods

Microstructural elucidation of self-emulsifying system: effect of chemical structure

Patil, S.S., Venugopal, E., Bhat, S., Mahadik, K.R., Paradkar, Anant R

January 2012

No / PURPOSE: Self-emulsifying systems (SES) emulsify spontaneously to produce fine oil-in-water emulsion when introduced into aqueous phase. The self-emulsification process plays an important role during formation of emulsion. The objective of current work was to understand and explore the inner structuration of SES through controlled hydration and further to study the influence of additive on the same which ultimately governs performance of final formulation in terms of droplet size. METHODS: Droplet size of final formulations containing structural analogues of ibuprofen was determined. Microstructural properties of intermediate hydrated regimes of SES were investigated using techniques such as small angle X-ray scattering, differential scanning calorimetry and rheology. RESULTS: The current work established inverse relationship between droplet size of the formulations containing structural analogues of ibuprofen and their Log P values. Microstructural analysis of intermediate hydrated regimes of the prepared samples showed formation of local lamellar structure. Structural analogues of ibuprofen significantly altered microstructure of lamellae which was well correlated with the droplet size of final formulations. In vitro drug release study showed increase in dissolution rate of lipophillic drugs when formulated as SES. CONCLUSION: The current work emphasizes the fact that tailor-made formulations can be prepared by controlling the properties of intermediate regimes.

Analgesics

Calorimetry

Diffusion

Emulsions

Ibuprofen

Oils

Particle size

Pharmaceutical vehicles

Rheology

Scattering

Solubility

Surface-active agents

Water

X-Ray diffraction

REF 2014

Non-Narcotic

Administration & dosage

Chemistry

Differential scanning

Flurbiprofen

Analogs & derivatives

Ketoprofen

Lamellar structure

Small angle

Comparing Immune Responses to Inactivated Vaccines Against SARS-CoV-2 Between People Living With HIV and HIV-Negative Individuals: A Cross-Sectional Study in China

Huang, Xiaojie, Yan, Ying, Su, Bin, Xiao, Dong, Yu, Maohe, Jin, Xia, Duan, Junyi, Zhang, Xiangjun, Zheng, Shimin, Fang, Yuan, Zhang, Tong, Tang, Weiming, Wang, Lunan, Wang, Zixin, Xu, Junjie

28 January 2022

This study compared the immunogenicity of inactivated SARS-CoV-2 vaccines between people living with HIV (PLWH) and HIV-negative individuals. We recruited 120 PLWH and 53 HIV-negative individuals aged 18-59 years who had received an inactivated SARS-CoV-2 vaccine in two Chinese cities between April and June 2021. Blood samples were tested for immunogenicity of the inactivated SARS-CoV-2 vaccines. The prevalence and severity of adverse events associated with SARS-CoV-2 vaccines were similar between PLWH and HIV-negative individuals. The seropositivity of neutralizing activity against authentic SARS-CoV-2, of the total amount of antibody (total antibody) and of S-IgG were 71.3%, 81.9%, and 92.6%, respectively, among fully vaccinated PLWH. Among all participants, PLWH had lower neutralizing activity, total antibody, S-IgG, and T-cell-specific immune response levels, compared to HIV-negative individuals, after controlling for types of vaccine, time interval between first and second dose, time after receiving the second dose, and sociodemographic factors. PLWH with a longer interval since HIV diagnosis, who received their second dose 15-28 days prior to study commencement, and who had an interval of ≥21 days between first and second dose had higher neutralizing activity levels. The immunogenicity of the inactivated SARS-CoV-2 vaccines was lower among PLWH as compared to HIV-negative individuals. Vaccination guideline specific for PLWH should be developed.

SARS-CoV-2 IgG antibody

antigen-specific T-cell immune response

inactivated SARS-CoV-2 vaccines

people living with HIV

self-reported adverse events

total antibody specific to SARS-CoV-2

adolescent

adult

antibodies

neutralizing (blood)

antibodies

viral (blood)

COVID-19 (epidemiology

immunology

prevention & control)

immunology)

China (epidemiology)

cross-sectional studies

female

HIV infections (complications

epidemiology

immunology)

humans

immunogenicity

vaccine

male

middle aged

vaccination

vaccines

inactivated (administration & dosage

immunology)

young adult

Biostatistics and Epidemiology

Analgesia preemptiva do cetoprofeno e do parecoxibe em cirurgia para remoção de terceiros molares inclusos / Preemptive analgesia of the ketoprofen and parecoxib in the surgery to removal of impacted third molar teeth

Arantes, Viviana Moraes Neder

03 October 2006

Este trabalho prospectivo, duplo-cego randomizado, avaliou o efeito da analgesia preemptiva do cetoprofeno e do parecoxibe. Sessenta pacientes foram submetidos à cirurgia para remoção de terceiros molares inferiores bilaterais inclusos, sendo operado um lado de cada vez. O paciente foi seu próprio controle. Os pacientes foram separados em dois grupos de 30 pacientes. No grupo parecoxibe, na primeira operação foi usado o parecoxibe ou placebo, endovenoso, 30 minutos antes da cirurgia e imediatamente após a operação foi feita a administração do placebo ou parecoxibe, garantindo ao paciente receber parecoxibe antes ou após a operação. O lado oposto foi operado após duas semanas da primeira cirurgia e o paciente que havia recebido parecoxibe antes e placebo depois da operação recebeu placebo antes e parecoxibe depois da operação e o que havia recebido placebo antes e parecoxibe depois recebeu parecoxibe antes e placebo depois. Nos 30 pacientes do grupo cetoprofeno, o modelo foi o mesmo, substituindo-se apenas o parecoxibe pelo cetoprofeno. O paciente pôde utilizar como medicação resgate a dipirona, sempre que necessário para controlar a dor pós-operatória. Após a operação foi fornecido para todos os pacientes um questionário, contendo a escala analógica visual (EAV), a escala descritiva de dor (EDD) e uma tabela para informar o consumo de medicação resgate. Foi avaliada a dor pós-operatória por meio da EAV, da EDD e pelo consumo de medicação resgate. Não houve diferença estatisticamente relevante quanto a intensidade da dor com o uso do parecoxibe ou do cetoprofeno antes ou depois do procedimento cirúrgico. Ao comparar a analgesia proporcionada pelo cetoprofeno e pelo parecoxibe os resultados mostraram que o parecoxibe administrado antes do procedimento cirúrgico foi mais eficaz do que o cetoprofeno no controle da dor na quarta hora do pós-operatório (p=0,041), mas foi menos eficaz após 24h (p=0,003). Quando se comparou a analgesia proporcionada por esses fármacos usados após a operação, o parecoxibe foi mais eficaz do que o cetoprofeno após 6 e 8h do procedimento (p=0,003 e 0,023, respectivamente). / This is a prospective, double-blind randomized, cross over experiment, to evaluate the effect of the preemptive analgesia of ketoprofen and parecoxib. Sixity patients who had gone though surgery for removal of the impacted mandibular bilateral third molar teeth, having one side operated each time, were evaluated. The patients were separated in groups of 30, in the parecoxib group (P). On the first operation parecoxib or placebo were used 30 minutes before the surgery. Immediately after the operation, placebo or parecoxib were administred, so that the patient who had received parecoxib before the operation or after it. The opposite side was operated two weeks after the first surgery and the patients who received parecoxib before and placebo after operation received placebo before and parecoxib after operation and patients who received placebo before and parecoxib after received parecoxib before and placebo after, under the same method. In the group C (n= 30), the model was the same, using ketoprofen instead parecoxib. The patient could use dipyrone as rescue medication, in the event of postoperative pain. A questionnaire was provided to the patient after each surgery, containing a visual analogic scale, a descriptive pain scale and a table to inform the consum of rescue medication. The postoperative pain was evaluated by visual analogic scale, descriptive pain scale and rescue medicine consum. There was no statistically relevant difference as pain intensity with use of parecoxib or ketoprofen before or after the surgical procedure. Comparing ketoprofen analgesia against parecoxib analgesial, the results shown that the administration of parecoxib before the surgical procedure had a major efficacy than ketoprofen in pain control by the fourth hour post operatory (p=0,041), but was less efficient after 24 hours (p=0,003). When comparing the analgesic effect of both drugs after the operation, parecoxib was more effective than ketoprofen six and eight hours after the procedure (p=0,003 and 0,023, respectively).

Analgesia/methods

Analgesia/métodos

Cetoprofeno/administração e dosagem

Cetoprofeno/uso terapêutico

Comparative study

Dor pós-operatória/fisiopatologia

Dor pós-operatória/terapia

Estudo comparativo

Ketoprofen/administration and dosage

Ketoprofen/therapeutic use

Medição da dor/métodos

Molar third/surgery

Pain measurement/methods

Pain postoperative/physiopathology

Pain postoperative/therapy

Terceiro molar/cirurgia

N-acetilcisteína melhora os fenótipos renal e cardíaco e reduz o peso corpóreo em camundongos císticos deficientes em Pkd1 / N-acetylcysteine improves renal and cardiac phenotypes and reduces body weight in Pkd1-deficient cystic mice

Moyses, Zenaide Providello

13 December 2013

Estudos experimentais e clínicos amparam a participação do estresse oxidativo na progressão da doença renal na doença renal policística autossômica dominante (DRPAD). A administração do agente antioxidante N-acetilcisteína (NAC), por sua vez, apresenta efeitos benéficos em vários modelos animais de injúria renal. Neste estudo, utilizamos um camundongo cístico gerado por meio do cruzamento de uma linhagem portadora de um alelo floxed Pkd1 com outra que expressa nestin-Cre para avaliar os efeitos da NAC sobre um modelo ortólogo à DRPAD humana. O tratamento de longo prazo com NAC foi iniciado na concepção, nascimento, desmame ou oito semanas de idade, de modo a permitir a avaliação de seus efeitos em diferentes fases da vida. Nossas análises revelaram que a administração de NAC reduziu o nível de substâncias reativas com ácido tiobarbitúrico e aumentou o de glutationa nos rins de camundongos císticos tratados com NAC desde a concepção (Ci-NAC-Conc) comparados a animais císticos não tratados (Ci-Co). A excreção urinária de óxido nítrico também foi maior em camundongos císticos tratados com NAC. Animais Ci-NAC-Conc apresentaram ureia sérica, número de cistos renais, índice cístico e fibrose intersticial renal mais baixos que os camundongos Ci-Co. Animais Ci-NAC-Conc apresentaram, além disso, fração de ejeção e fração de encurtamento de ventrículo esquerdo maiores que camundongos Ci-Co, assim como menor fibrose cardíaca. O tratamento com NAC iniciado na concepção aumentou a sobrevida dos animais císticos. Notavelmente, o peso corpóreo mostrou-se significantemente menor em camundongos Ci-NAC-Conc que nos animais Ci-Co em todas as idades avaliadas, uma diferença não observada entre animais não císticos tratados e não tratados com NAC. Ainda é incerto se todas as ações observadas da NAC são causadas por suas propriedades antioxidantes. Esses resultados apóiam efeitos benéficos de tratamento precoce com NAC em camundongos císticos deficientes em Pkd1, determinados pela melhora de seus fenótipos renal, cardíaco e sistêmico. Nossos achados também revelam uma redução não deletéria no crescimento corpóreo, induzida pela administração de longo prazo de NAC no background deficiente em Pkd1 avaliado. Nossos dados abrem uma linha de pesquisa significativa e provavelmente robusta para se intervir nos fenótipos renal, cardíaco e sistêmico da DRPAD / Oxidative stress has been postulated to participate in the progression of renal disease in autosomal dominant polycystic kidney disease (ADPKD). The antioxidant N-acetylcysteine (NAC), in turn, has been shown to determined beneficial effects on several animal models of renal injury. In the current study, a cystic mouse generated by breeding a Pkd1 floxed allele with a nestin Cre expressing line was used to evaluate the potential therapeutic effects of NAC on a model orthologous to human ADPKD. Long-term NAC treatment was initiated at conception, birth, weaning or 8 weeks of life, to allow the evaluation of its effects on different phases of life. Our analyses revealed that NAC decreased thiobarbituric acid reactive substances (TBARS) and increased glutathione levels in the kidneys of mice treated with NAC since conception (CY-NAC-Con) compared with non-treated cystic animals (CY-Ctl). Nitric oxide urinary excretion was also higher in NAC-treated cystic mice. These animals showed lower serum urea nitrogen (SUN), number of renal cysts, cystic index and renal interstitial fibrosis than CY-Ctl mice. CY-NAC-Con animals displayed, in addition, higher left ventricle ejection fraction and fractional shortening compared with CY-Ctl mice, as well as decreased cardiac fibrosis. NAC treatment started at conception increased the survival of cystic mice, demonstrating beneficial systemic effects. Interestingly, body weight was significantly lower in CY-NAC-Con than CY-Ctl mice at all evaluated times, a difference not observed between non-cystic animals treated and not treated with NAC Whether all observed NAC actions are caused by its antioxidant properties is yet not clear. These results support beneficial effects of early treatment with NAC on Pkd1-deficient cystic mice, by determining improvement in their renal, heart and systemic phenotypes. Our findings also reveal a non-deleterious reduction in body growth induced by long-term NAC administration in the evaluated Pkd1-deficient background. Our data open a likely significant and robust research track to intervene in renal, extra-renal and systemic ADPKD phenotypes

Acetylcysteine/administration e dosage

Análise de sobrevida

Body weight

Camundongos

Depuradores de radicais livres

Doenças renais císticas

Estresse oxidativo

Fenótipo

Fibrose

Fibrosis

Free radical scavengers

Kidney diseases cystic

Mice

Modelos animais

Models animal

Oxidative stress

Peso corporal

Phenotype

Survival analysis