MUO

MUO
  • 文章类型: Journal Article
    背景:缺乏与病因不明的脑膜脑炎(MUE)幼犬的结局有关的信息。
    目的:描述临床表现,诊断结果,治疗,和结果在MUE<52周龄的狗队列中。
    方法:34只客户拥有的狗。
    方法:多中心回顾性病例系列。检索了5个转诊中心的记录。从医疗记录中提取数据,如果无法从记录中获得生存数据,则联系转诊的兽医。
    结果:平均年龄为31周;最小的狗为11周,3只狗<16周大。改变状态(71%),共济失调(44%),缉获量(29%),和盘旋(26%)是最常见的投诉。神经解剖定位在前脑(38%),多焦(35%),脑干(18%),和小脑(12%)。以相等比例使用皮质类固醇单一疗法(n=15)和皮质类固醇加胞嘧啶阿拉伯糖苷(n=15)。有26只狗的结果数据,8(31%)在数据收集时存活,随访范围为135至2944天。在研究期间死亡的17/18只狗中,死亡或安乐死与MUE有关。Kaplan-Meier生存分析显示全因死亡的中位生存时间为84天。
    结论:该亚组犬的MUE预后较差。
    BACKGROUND: The information relating to the outcome specifically for juvenile dogs with meningoencephalitis of unknown etiology (MUE) is lacking.
    OBJECTIVE: To describe the clinical presentation, diagnostic findings, treatment, and outcome in a cohort of dogs with MUE <52 weeks old.
    METHODS: Thirty-four client-owned dogs.
    METHODS: Multicenter retrospective case series. Records from 5 referral centers were searched. Data was extracted from the medical records and referring veterinarians were contacted for survival data if this was not available from the record.
    RESULTS: The mean age was 31 weeks; the youngest dog was 11 weeks and 3 dogs were <16 weeks old. Altered mentation (71%), ataxia (44%), seizures (29%), and circling (26%) were the most common presenting complaints. Neuroanatomical localization was to the forebrain (38%), multifocal (35%), brainstem (18%), and cerebellum (12%). Corticosteroid monotherapy (n = 15) and corticosteroid plus cytosine arabinoside (n = 15) were used in equal proportions. Outcome data was available for 26 dogs, 8 (31%) were alive at the time of data collection with a follow-up range of 135 to 2944 days. Death or euthanasia was related to MUE in 17/18 dogs that died during the study period. Kaplan-Meier survival analysis demonstrated a median survival time for all-cause death of 84 days.
    CONCLUSIONS: The prognosis for MUE in this subset of dogs was considered poor.
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  • 文章类型: Case Reports
    一只2.5岁的雌性波美拉尼亚犬因急性轻瘫在2天内进展为截瘫。一般体格检查不明显。神经系统检查显示截瘫无伤害性感受,在骨盆四肢和髌骨反射亢进中测试会阴反射和退缩反射时的质量反射。第六胸椎水平的尾端没有皮肤干反射。存在脊髓感觉过敏。神经解剖定位与T3-L3脊髓病一致。血液学和生化血液检查[包括C反应蛋白(CRP)]在参考范围内。从第一胸椎水平到骶骨的脊髓MRI显示有斑片状,不明确,中度至显著的T2W高强度,对比增强髓内病变从T1延伸到L4。基于疼痛评分的皮质类固醇和美沙酮开始基于未知原因的脑膜脊髓炎的工作诊断的药物治疗。预后严重,3天后无伤害性感觉复发,根据主人的意愿对狗实施了安乐死。大脑和脊髓的死后组织病理学检查产生了严重的形态学诊断,分段,双边且相当对称,坏死性淋巴组织细胞性白血病,患有非化脓性血管中心性软脑膜炎。一些未成年人,焦点,在延髓中也发现了淋巴细胞血管周围袖套,但除此之外没有大脑受累的迹象.辅助测试未发现感染原因。此病例报告强调了将脑膜脊髓炎纳入有关脊髓病的急性进行性神经系统体征的犬的鉴别诊断列表中的重要性。
    A 2.5-year-old female entire Pomeranian dog was presented for acute paraparesis progressing within 2 days to paraplegia. General physical examination was unremarkable. Neurological examination showed paraplegia without nociception, a mass reflex upon testing perineal reflexes and withdrawal reflexes in the pelvic limbs and patellar hyperreflexia. Cutaneous trunci reflexes were absent caudal to the level of the 6th thoracic vertebra. Spinal hyperesthesia was present. Neuroanatomical localization was consistent with a T3-L3 myelopathy. Hematological and biochemical blood tests [including C-reactive protein (CRP)] were within reference ranges. MRI of the spinal cord from the level of the 1st thoracic vertebra to the sacrum revealed a patchy, ill-defined, moderate to marked T2W hyperintense, contrast enhancing intramedullary lesion extending from T1 to L4. Medical treatment based on a working diagnosis of meningomyelitis of unknown cause was initiated with corticosteroids and methadone based on pain scores. Prognosis was grave and after 3 days without return of nociception, the dog was euthanized according to the owners\' wishes. Post-mortem histopathological examination of the brain and spinal cord yielded a morphological diagnosis of severe, segmental, bilateral and fairly symmetrical, necrotizing lymphohistiocytic leukomyelitis, with a non-suppurative angiocentric leptomeningitis. Some minor, focal, lymphocytic perivascular cuffing was found in the medulla oblongata as well, but otherwise there were no signs of brain involvement. No infectious causes were identified with ancillary tests. This case report underlines the importance of including meningomyelitis in the differential diagnosis list of dogs presented for acute progressive neurological signs referable to a myelopathy.
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  • 文章类型: Journal Article
    背景:不明原因脑膜脑炎(MUO)包括一组影响犬中枢神经系统的非感染性炎症性疾病。先前的研究已经报道了生存的个体风险因素,但MUO的预测仍然具有挑战性。
    目的:确定MUO犬的临床预后变量。
    方法:一项回顾性研究,纳入英国2家转诊医院并诊断为MUO的447只狗。
    方法:回顾性分析诊断为MUO的犬的病历。多变量logistic回归用于确定生存的危险因素,Cox比例风险分析用于确定临床复发的危险因素。
    结果:82%(366/447)的推定MUO犬存活至出院,63.5%(284/447)在6个月时存活;后者的36%(103/284)具有持续的神经功能缺损。品种(哈巴狗;P=.03),癫痫发作(P<.001),轻瘫(P<.001),和较高的神经残疾量表(NDS)评分(P<.001)与6个月的生存期呈负相关。具有持续性缺陷的狗在表现时具有较高的NDS得分(P=.001)。中位随访时间为11个月(四分位距[IQR],1-24)和50.6%(160/316)在治疗期间复发(中位复发时间,7个月;IQR,2-15).诊断后6个月临床体征不完全消退(P<.001),较高的NDS评分(P<.001),临床体征持续时间较长(P<.001)与复发有关。
    结论:了解与生存相关的危险因素,MUO的不完全康复和临床复发可以帮助指导监测和治疗,并改善所有者关于这种使人衰弱的疾病预后的沟通。
    BACKGROUND: Meningoencephalitis of unknown origin (MUO) comprises a group of noninfectious inflammatory diseases affecting the central nervous system of dogs. Previous studies have reported individual risk factors for survival but prognostication for MUO remains challenging.
    OBJECTIVE: Identify clinical prognostic variables in dogs with MUO.
    METHODS: A retrospective study of 447 dogs presented to 2 UK referral hospitals and diagnosed with MUO.
    METHODS: Medical records of dogs diagnosed with MUO were retrospectively reviewed. Multivariable logistic regression was used for the identification of risk factors for survival and Cox proportional hazards analysis for the identification of risk factors for clinical relapse.
    RESULTS: Eighty-two percent (366/447) of dogs with presumptive MUO survived to discharge and 63.5% (284/447) were alive at 6 months; 36% of the latter (103/284) had persistent neurological deficits. Breed (pugs; P = .03), epileptic seizures (P < .001), paresis (P < .001), and higher neurodisability scale (NDS) score (P < .001) at presentation were negatively associated with survival to 6 months. Dogs with persistent deficits had higher NDS scores on presentation (P = .001). Median follow-up time was 11 months (interquartile range [IQR], 1-24) and 50.6% (160/316) relapsed during treatment (median time to relapse, 7 months; IQR, 2-15). Incomplete resolution of the clinical signs during the 6 months after diagnosis (P < .001), higher NDS score (P < .001), and longer duration of the clinical signs (P < .001) were associated with relapse.
    CONCLUSIONS: Knowledge of risk factors associated with survival, incomplete recovery and clinical relapse in MUO can help guide monitoring and treatment and improve owner communications regarding prognosis for this debilitating disease.
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  • 文章类型: Journal Article
    未知起源的犬脑膜脑炎(MUO)是一种与高死亡率相关的使人衰弱的疾病。磁共振成像(MRI)结果预测12个月生存率和长期复发的预后价值仍不确定。
    这是一项回顾性队列研究,使用多变量逻辑回归和Cox比例风险分析评估不同MRI变量的预后价值。
    总共,138只狗被推定诊断为MUO。在MRI上确定的病变最常见的位置是放射状电晕和call体的白质束,紧随其后的是额叶,感觉运动和颞叶皮质。较低的T2病变负荷(p=0.006,OR=0.942,CI=0.902-0.983)与较长的生存期相关,而较高的T1造影后病变负荷(p=0.023,OR=1.162,CI=1.021-1.322)与复发相关。
    这项研究确定了预后因素,这些因素可能有助于识别死亡和复发风险较高的狗,从而指导治疗建议。
    UNASSIGNED: Canine meningoencephalitis of unknown origin (MUO) is a debilitating disease associated with high mortality. The prognostic value of magnetic resonance imaging (MRI) findings for predicting survival at 12 months and long-term relapse remains uncertain.
    UNASSIGNED: This was a retrospective cohort study evaluating the prognostic value of different MRI variables using multivariable logistic regression and Cox proportional hazards analysis.
    UNASSIGNED: In total, 138 dogs were presumptively diagnosed with MUO. The most common location for lesions identified on MRI were the white matter tracts of the corona radiata and corpus callosum, followed by the frontal, sensorimotor and temporal cortices. Lower T2 lesion load (p = 0.006, OR = 0.942, CI = 0.902-0.983) was associated with longer survival and higher T1 post-contrast lesion load (p = 0.023, OR = 1.162, CI = 1.021-1.322) was associated with relapse.
    UNASSIGNED: This study has identified prognostic factors that may help identify dogs at higher risk of death and relapse and therefore guide treatment recommendations.
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  • 文章类型: Journal Article
    这项研究调查了性别差异对大量营养素数量的影响,质量,以及代谢不健康的超重/肥胖(MUO)人群的死亡率时间。这项研究包括18,345名参与者,包括9204名男性和9141名女性。Cox比例风险模型和等热量替代效应用于检查MUO人群中大量营养素摄入量和亚型与全因死亡率的关系。在调整潜在协变量后,与最低四分位数的男性相比,不良碳水化合物含量最高的25%百分位的男性全因死亡风险升高(比值比[OR]:2.04;95%置信区间[CI],1.40-2.98)。与最低四分位数的女性相比,优质碳水化合物(OR:0.74;95%CI,0.55~0.99)和不饱和脂肪酸(OR:0.54;95%CI,0.32~0.93)占25%百分位数最高的女性全因死亡率风险降低.在女性中,在等热量基础上用高质量碳水化合物代替低质量碳水化合物可将全因死亡风险降低约9%.我们发现不同的常量营养素消费亚型与MUO人群的全因死亡率相关。男女之间有不同的影响,全因死亡的风险受大量营养素质量和进餐时间的影响。
    This study investigates sex differences in the effects of macronutrient quantity, quality, and timing on mortality in metabolically unhealthy overweight/obesity (MUO) populations. The study included 18,345 participants, including 9204 men and 9141 women. The Cox proportional risk model and isocaloric substitution effects were used to examine the association of macronutrient intake and subtype with all-cause mortality in the MUO populations. After adjusting for the potential covariates, The risk of all-cause mortality was elevated in men in the highest 25% percentile of poor-quality carbohydrates compared with men in the lowest quartile (odds ratio [OR]: 2.04; 95% confidence interval [CI], 1.40-2.98). Compared with women in the lowest quartile, the risk of all-cause mortality for women in the highest 25% percentile for high-quality carbohydrates (OR: 0.74; 95% CI, 0.55-0.99) and unsaturated fatty acids (OR: 0.54; 95% CI, 0.32-0.93) were decreased. In women, replacing low-quality carbohydrates with high-quality carbohydrates on an isocaloric basis reduces the risk of all-cause mortality by approximately 9%. We find that different macronutrient consumption subtypes are associated with all-cause mortality in MUO populations, with differential effects between men and women, and that the risk of all-cause mortality is influenced by macronutrient quality and meal timing.
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  • 文章类型: Journal Article
    目的:恶性输尿管梗阻是一个重大的治疗挑战。输尿管支架的失败通常会导致长期的肾造瘘管。由于其相关的发病率,这会尽可能长时间地延迟。有几种类型的输尿管支架,然而,几乎没有证据表明哪种支架能更好地预防肾造瘘管的进展.这项研究旨在确定新的6French(Fr)聚合物支架,一旦初始聚合物输尿管支架失效,8Fr聚合物支架或金属支架实现更长的功能持续时间。
    方法:回顾性研究,纵向研究是在一家高等教育机构进行的.纳入了2010年至2020年期间使用6Fr聚合物支架进行输尿管支架置入术治疗恶性肿瘤的所有患者。对患者进行原位输尿管支架或永久性肾造瘘管插入随访直至死亡。
    结果:共有46例患者(66个输尿管)植入了用于治疗恶性肿瘤的输尿管支架。从最初的输尿管支架失败开始,10个支架改为新的6Fr聚合物支架,将42个改为8Fr聚合物支架,并将14个改为Resonance®6Fr金属支架。共振6Fr金属支架的中位功能持续时间最长为14个月(p=0.012)。
    结论:与新的6Fr聚合物支架或8Fr聚合物支架相比,Resonance®6Fr金属支架的功能持续时间明显更长,这可能使患者享受更好的生活质量,并延迟永久性肾造瘘管的插入。
    OBJECTIVE: Malignant ureteric obstruction is a significant management challenge. The failure of ureteric stents often leads to long-term nephrostomy tubes. This is delayed for as long as possible due to its\' associated morbidity. Several types of ureteric stents are available, however there is little evidence demonstrating which stents are better for preventing progression to nephrostomy tubes. This study looked to determine whether a new 6 French (Fr) polymer stent, 8Fr polymer stent or metallic stent achieved a longer functional duration once the initial polymer ureteric stent failed.
    METHODS: A retrospective, longitudinal study was performed at a single tertiary institution. All patients who underwent ureteric stenting with a 6Fr polymer stent for malignancy between 2010 and 2020 were included. Patients were followed up until death with ureteric stent in situ or permanent nephrostomy tube insertion.
    RESULTS: A total of 46 patients (66 ureters) had ureteric stents inserted for malignancy. From initial ureteric stent failure, 10 stents were changed to a new 6Fr polymer stent, 42 were changed to an 8Fr polymer stent and 14 were changed to a Resonance® 6Fr metallic stent. The Resonance 6Fr metallic stent had the longest median functional duration of 14 months (p = 0.012).
    CONCLUSIONS: Resonance® 6Fr metallic stents appear to have a significantly longer functional duration than a new 6Fr polymer stent or 8Fr polymer stent, which may allow patients to enjoy a better quality of life and delay permanent nephrostomy tube insertion.
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  • 文章类型: Journal Article
    在这次审查中,我们深入研究了肥胖中白色脂肪组织(WAT)重塑和代谢方面之间的复杂关系,特别关注代谢健康肥胖(MHO)和代谢不健康肥胖(MUO)的个体。WAT是一个高度异质的,塑料,动态分泌内分泌和免疫器官。WAT重塑在代谢健康中起着至关重要的作用,涉及扩展模式,微环境,表型,和分配。在拥有MHO的个人中,WAT重塑是有益的,通过增加脂肪细胞增生等机制减少异位脂肪沉积和胰岛素抵抗(IR),抗炎微环境,适当的细胞外基质(ECM)重塑,适当的血管化,增强WAT褐变,和皮下脂肪组织(SWAT)沉积。相反,对于那些有MUO的人来说,WAT重塑导致异位脂肪沉积和IR,导致代谢失调.这个过程涉及脂肪细胞肥大,血管化中断,促炎微环境增强,增强棕色脂肪组织(BAT)美白,和内脏脂肪组织(VWAT)沉积的积累。审查强调了干预WAT改造以阻碍从MHO向MUO过渡的重要性。这种见解对于在临床实践中为肥胖患者量身定制个性化和有效的管理策略很有价值。
    In this review, we delve into the intricate relationship between white adipose tissue (WAT) remodeling and metabolic aspects in obesity, with a specific focus on individuals with metabolically healthy obesity (MHO) and metabolically unhealthy obesity (MUO). WAT is a highly heterogeneous, plastic, and dynamically secreting endocrine and immune organ. WAT remodeling plays a crucial role in metabolic health, involving expansion mode, microenvironment, phenotype, and distribution. In individuals with MHO, WAT remodeling is beneficial, reducing ectopic fat deposition and insulin resistance (IR) through mechanisms like increased adipocyte hyperplasia, anti-inflammatory microenvironment, appropriate extracellular matrix (ECM) remodeling, appropriate vascularization, enhanced WAT browning, and subcutaneous adipose tissue (SWAT) deposition. Conversely, for those with MUO, WAT remodeling leads to ectopic fat deposition and IR, causing metabolic dysregulation. This process involves adipocyte hypertrophy, disrupted vascularization, heightened pro-inflammatory microenvironment, enhanced brown adipose tissue (BAT) whitening, and accumulation of visceral adipose tissue (VWAT) deposition. The review underscores the pivotal importance of intervening in WAT remodeling to hinder the transition from MHO to MUO. This insight is valuable for tailoring personalized and effective management strategies for patients with obesity in clinical practice.
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  • 文章类型: Journal Article
    背景:不明原因的脑膜脑炎是狗严重神经系统疾病的常见原因。该术语涵盖一组异质性的非感染性炎性疾病,免疫失调被广泛认为是潜在的疾病机制。目前的治疗包括免疫抑制,皮质类固醇是几乎所有治疗方案的支柱。然而,皮质类固醇的副作用可能很严重,可能是一些病人的死因.这次回顾,多中心研究旨在描述斯堪的纳维亚犬群患有未知来源的脑膜脑炎,关于报告的副作用和死亡原因,并强调可能的生存差异,当比较皮质类固醇单一疗法与其他治疗方案时。
    结果:在5年的研究期内,包括63只狗。其中,35人(49.3%)在研究期间死亡或被安乐死。根据Kaplan-Meier曲线,从诊断时间开始的中位生存时间为714天(相当于约25个月,范围0-1678天)。用皮质类固醇单一疗法治疗的狗之间的生存率没有统计学上的显着差异(P=0.31)(n=26,中位生存时间716天,相当于25个月左右,范围5-911天),接受皮质类固醇和环孢素组合的狗(n=15,中位生存时间916天,相当于31个月左右,范围35-1678天),接受皮质类固醇联合阿糖胞苷的狗,来氟米特,或2种或更多种附加药物的组合(n=13,中位生存时间1186天,相当于大约40个月,范围121-1640天)。对47/63只狗进行了副作用记录。多食(n=37/47),多尿/多饮(n=37/47),腹泻(n=29/47)和嗜睡(n=28/47)最常见.安乐死最常见的原因是复发(n=15/35,42.9%),其次是治疗反应不足或缺乏(n=9,25.7%)。副作用是2/35犬(5.7%)安乐死的直接原因。
    结论:总体人群中很大比例的狗因复发而被安乐死,强调需要专门预防复发以改善长期生存率的治疗方案。接受皮质类固醇单一疗法的狗的副作用很少是直接死亡原因,但所有的狗都有报道。当皮质类固醇单药治疗与其他治疗方案相比时,没有发现统计学上的显着差异。
    BACKGROUND: Meningoencephalitis of unknown origin is a common cause of severe neurological disease in dogs. The term covers a heterogeneous group of noninfectious inflammatory diseases, with immune dysregulation widely accepted as the underlying disease mechanism. Current treatment consists of immunosuppression, with corticosteroids being the mainstay of virtually all treatment regimens. However, side effects of corticosteroids can be severe, and might be the cause of death in some patients. This retrospective, multi-centric study aimed at describing a population of Scandinavian dogs with meningoencephalitis of unknown origin in regards to reported side effects and cause of death, and to highlight possible differences in survival, when comparing corticosteroid monotherapy with other treatment regimens.
    RESULTS: Within the 5-year study period, 63 dogs were included. Of these, 35 (49.3%) died or were euthanized during the study period. Median survival time from time of diagnosis based on Kaplan-Meier curves for the overall population was 714 days (equivalent to around 25 months, range 0-1678 days). There was no statistically significant difference (P = 0.31) in survival between dogs treated with corticosteroid monotherapy (n = 26, median survival time 716 days, equivalent to around 25 months, range 5-911 days), dogs receiving a combination of corticosteroids and ciclosporin (n = 15, median survival time 916 days, equivalent to around 31 months, range 35-1678 days), and dogs receiving corticosteroids combined with either cytosine arabinoside, leflunomide, or a combination of 2 or more add-on drugs (n = 13, median survival time 1186 days, equivalent to around 40 months, range 121-1640 days). Side effects were registered for 47/63 dogs. Polyphagia (n = 37/47), polyuria/polydipsia (n = 37/47), diarrhea (n = 29/47) and lethargy (n = 28/47) were most frequently reported. The most common cause for euthanasia was relapse (n = 15/35, 42.9%), followed by insufficient or lack of treatment response (n = 9, 25.7%). Side effects were the direct cause of euthanasia in 2/35 dogs (5.7%).
    CONCLUSIONS: A large proportion of dogs in the overall population were euthanized due to relapse, emphasizing a need for treatment regimens aimed at specifically preventing relapse for an improved long-term survival. Side effects in dogs receiving corticosteroid monotherapy were rarely a direct cause of death, but were reported for all dogs. No statistically significant difference in survival was found when corticosteroid monotherapy was compared to other treatment regimens.
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  • 文章类型: Observational Study
    背景:术语代谢健康肥胖(MHO)和代谢不健康肥胖(MUO)根据心脏代谢危险因素的存在或不存在对肥胖受试者进行分类。由于心脏代谢并发症的高风险,检测MUO表型至关重要,需要量身定制和密集的后续行动。然而,诊断MUO是耗时且昂贵的。因此,我们旨在研究地中海饮食(MD)在确定MHO/MUO表型中的作用,以及坚持MD是否可作为MUO表型的额外筛查工具.
    方法:这项横断面观察研究的研究人群包括275名肥胖受试者。我们评估了他们的生活习惯(体力活动和吸烟习惯),人体测量(体重,高度,腰围,体重指数),血压,代谢参数,炎症标志物(高敏C反应蛋白水平),对MD的依从性(通过PREvenciónCONDIetaMEDiterránea(PREDIMED)问卷),和MHO/MUO表型。
    结果:该研究包括275名肥胖个体(256F/19M;34.0±10.5岁;BMI38.3±5.95kg/m2)。其中,114(41.5%)表现为MHO表型,161人(58.5%)具有MUO表型。MHO表型表现出良好的人体测量和心脏代谢谱,以腰围较低(p<0.001)为特征,BMI(p<0.001),胰岛素抵抗(p<0.001),血压(p<0.001),炎症(p<0.001),和脂质水平(p<0.001)与MUO表型相比。值得注意的是,我们发现,MHO表型有较高的坚持MD(p<0.001)和消耗更多的特级初榨橄榄油(EVOO)(p<0.001),蔬菜(p<0.001),水果(p<0.001),豆类(p=0.001),鱼(p<0.001),葡萄酒(p=0.008),和坚果(p=0.001),虽然报告红色/加工肉类的摄入量较低(p<0.001),黄油,奶油,人造黄油(p=0.008),汽水饮料(p=0.006),和商业糖果(p=0.002)与MUO表型相比。坚持MD(p<0.001)和EVOO(p=0.015)摄入被认为是确定MUO/MHO表型存在的影响因素。此外,前评分<5被证明是预测MUO表型存在的最敏感和特异性的切点值(p<0.001)。
    结论:对MD的高依从性与MHO表型相关。此外,我们建议,PREDIMED评分的特定截止值可能是区分MUO/MHO表型患者的一个指标,因此有助于识别需要特定饮食干预的心血管风险较高的患者.
    The terms metabolically healthy obesity (MHO) and metabolically unhealthy obesity (MUO) categorize subjects with obesity based on the presence or absence of cardio-metabolic risk factors. Detecting MUO phenotype is crucial due to the high risk of cardio-metabolic complications, requiring tailored and intensive follow-up. However, diagnosing MUO is time-consuming and costly. Thus, we aimed to investigate the role of Mediterranean diet (MD) in determining MHO/MUO phenotypes and whether adherence to MD could serve as an additional screening tool for MUO phenotype.
    The study population of this cross-sectional observational study consisted of 275 subjects with obesity. We assessed their lifestyle habits (physical activity and smoking habits), anthropometric measurements (weight, height, waist circumference, body mass index), blood pressure, metabolic parameters, inflammatory marker (high sensitivity C reactive protein levels), adherence to MD (by PREvención con DIetaMEDiterránea (PREDIMED) questionnaire), and MHO/MUO phenotypes.
    The study included 275 individuals with obesity (256F/19M; 34.0 ± 10.5 years; BMI 38.3 ± 5.95 kg/m2). Among them, 114 (41.5%) exhibited MHO phenotype, while 161 (58.5%) had MUO phenotype. MHO phenotype exhibited favorable anthropometric and cardio-metabolic profiles, characterized by lower waist circumference (p < 0.001), BMI (p < 0.001), insulin resistance (p < 0.001), blood pressure (p < 0.001), inflammation (p < 0.001), and lipid levels (p < 0.001) compared to MUO phenotype. Notably, we found that MHO phenotype had higher adherence to MD (p < 0.001) and consumed more extra virgin olive oil (EVOO) (p < 0.001), vegetables (p < 0.001), fruits (p < 0.001), legumes (p = 0.001), fish (p < 0.001), wine (p = 0.008), and nuts (p = 0.001), while reporting lower intake of red/processed meats (p < 0.001), butter, cream, margarine (p = 0.008), soda drinks (p = 0.006), and commercial sweets (p = 0.002) compared to MUO phenotype. Adherence to MD (p < 0.001) and EVOO (p = 0.015) intake were identified as influential factors in determining the presence of MUO/MHO phenotypes. Furthermore, a PREDIMED score < 5 proved to be the most sensitive and specific cut-point value for predicting the presence of MUO phenotype (p < 0.001).
    High adherence to MD was associated with MHO phenotype. Moreover, we suggest that a specific cut-off of the PREDIMED score could be an indicator to discriminate patients with MUO/MHO phenotypes and therefore help in identifying patients at higher cardiovascular risk who will require specific dietary intervention.
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  • 文章类型: Journal Article
    类固醇反应性脑膜炎-动脉炎(SRMA)是一种主要的Th-2免疫介导的疾病,但确切的病理机制尚不清楚.白细胞介素-31(IL-31)主要由在促炎病症期间具有Th-2表型的T细胞产生。我们推测IL-31可能参与了SRMA的发病机制。在具有SRMA的狗的存档样品(49份血清和52份CSF样品)中测量IL-31,不明原因脑膜脑炎(MUO),感染性脑膜脑炎,和特应性皮炎,和使用竞争性犬IL-31ELISA的健康对照犬。与特应性皮炎犬(n=3,p=0.8135)和MUO犬(n=15,p=0.7618)相比,SRMA犬(n=18)的平均血清IL-31水平略高,并且明显高于健康对照(n=10,p=0.1327)和感染性脑膜脑炎犬(n=3,无统计)。在疾病的急性期并且没有任何预处理的具有SRMA的狗具有最高的IL-31水平。SRMA犬(n=23)的平均CSFIL-31值与健康对照组(n=8,p=0.4454)非常相似,与MUO犬(n=19,p=0.8724)和感染性脑膜脑炎。基于这项研究,IL-31参与SRMA中的全身性Th-2免疫介导的免疫应答的发病机理可以被认为是导致异常免疫反应的另一组分。
    Steroid-responsive meningitis-arteritis (SRMA) is a predominantly Th-2 immune-mediated disease, but the exact pathomechanism remains unclear. Interleukin-31 (IL-31) is predominantly produced by T cells with a Th-2 phenotype during proinflammatory conditions. We hypothesize that IL-31 might be involved in the pathogenesis of SRMA. IL-31 was measured in archived samples (49 serum and 52 CSF samples) of dogs with SRMA, meningoencephalitis of unknown origin (MUO), infectious meningoencephalitis, and atopic dermatitis, and of healthy control dogs using a competitive canine IL-31 ELISA. The mean serum IL-31 level in dogs with SRMA (n = 18) was mildly higher compared to dogs with atopic dermatitis (n = 3, p = 0.8135) and MUO (n = 15, p = 0.7618) and markedly higher than in healthy controls (n = 10, p = 0.1327) and dogs with infectious meningoencephalitis (n = 3, no statistics). Dogs with SRMA in the acute stage of the disease and without any pre-treatment had the highest IL-31 levels. The mean CSF IL-31 value for dogs with SRMA (n = 23) was quite similar to that for healthy controls (n = 8, p = 0.4454) and did not differ markedly from dogs with MUO (n = 19, p = 0.8724) and infectious meningoencephalitis. Based on this study, an involvement of IL-31 in the pathogenesis of the systemic Th-2 immune-mediated immune response in SRMA can be assumed as a further component leading to an aberrant immune reaction.
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