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Plasma protein-bound di-tyrosines as biomarkers of oxidative stress in end stage renal disease patients on maintenance haemodialysis 血浆蛋白结合二酪氨酸作为终末期肾病维持血液透析患者氧化应激的生物标志物
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2016.12.004
Graziano Colombo , Francesco Reggiani , David Cucchiari , Nicola M. Portinaro , Daniela Giustarini , Ranieri Rossi , Maria Lisa Garavaglia , Nicola Saino , Aldo Milzani , Salvatore Badalamenti , Isabella Dalle-Donne

Background

Patients with end-stage renal disease (ESRD) undergoing haemodialysis (HD) experience enhanced oxidative stress and systemic inflammation, which are risk factors for cardiovascular disease, the most common cause of excess morbidity and mortality for these patients. Different pathways producing different types of oxidative stress occur in ESRD. The purpose of our study was to determine the effect of HD on plasma levels of protein-bound dityrosine (di-Tyr), a biomarker of protein oxidation.

Methods

Protein-bound di-Tyr formation was measured by size exclusion HPLC coupled to fluorescence detector. Clinical laboratory parameters were measured by standardized methods.

Results

In most ESRD patients, a single HD session decreased significantly the plasma protein-bound di-Tyr level, although the mean post-HD level remained significantly greater than the one in healthy people. Furthermore, pre-HD plasma protein-bound di-Tyr level was positively correlated with pre-HD serum creatinine and albumin concentrations. No significant correlation was found between plasma protein-bound di-Tyr level and serum concentration of C-reactive protein, a biomarker of systemic inflammation.

Conclusions

This study demonstrates that a single HD session does not increase, rather partially decreases, oxidative pathways producing di-Tyr in the haemodialyzed patient.

General significance

The choice of the most pertinent biomarkers of oxidative stress is critical for the development of novel treatments for ESRD. However, the relative importance of oxidative stress and inflammation in ESRD remains largely undetermined, and several questions concerning oxidative stress and inflammation remain poorly defined. These results could stimulate further studies on the use of plasma protein-bound di-Tyr as a long-lasting oxidative stress biomarker in ESRD.

背景:接受血液透析(HD)的终末期肾病(ESRD)患者会经历氧化应激和全身性炎症的增强,这是心血管疾病的危险因素,也是这些患者发病率和死亡率过高的最常见原因。ESRD中产生不同类型氧化应激的途径不同。我们研究的目的是确定HD对血浆蛋白结合二酪氨酸(di-Tyr)水平的影响,二酪氨酸是一种蛋白质氧化的生物标志物。方法采用尺寸排除高效液相色谱法结合荧光检测器检测蛋白结合二酪氨酸的形成。采用标准化方法测定临床实验室参数。结果在大多数ESRD患者中,单次HD治疗显著降低血浆蛋白结合的di-Tyr水平,尽管HD后的平均水平仍显著高于健康人群。此外,hd前期血浆蛋白结合的di-Tyr水平与hd前期血清肌酐和白蛋白浓度呈正相关。血浆蛋白结合的di-Tyr水平与血清c反应蛋白(全身性炎症的生物标志物)浓度之间无显著相关性。结论:本研究表明,在血液透析患者中,单次HD治疗不会增加,反而会部分减少产生二tyr的氧化途径。选择最相关的氧化应激生物标志物对于开发ESRD的新治疗方法至关重要。然而,氧化应激和炎症在ESRD中的相对重要性在很大程度上仍未确定,有关氧化应激和炎症的几个问题仍未明确。这些结果可以刺激进一步研究血浆蛋白结合的二tyr作为ESRD中持久氧化应激生物标志物的使用。
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引用次数: 14
Microparticle subpopulations are potential markers of disease progression and vascular dysfunction across a spectrum of connective tissue disease 微粒亚群是结缔组织疾病进展和血管功能障碍的潜在标志
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2016.11.003
E.M. McCarthy , D. Moreno-Martinez , F.L. Wilkinson , N.J. McHugh , I.N. Bruce , J.D. Pauling , M.Y. Alexander , B. Parker

Objective

Microparticles (MPs) are membrane-bound vesicles derived from vascular and intravascular cells such as endothelial cells (EMPs) and platelets (PMPs). We investigated EMP and PMP numbers across a spectrum of autoimmune rheumatic diseases (AIRDs) with the aim of comparing the levels of, and relationship between, EMPs and PMPs.

Methods

Patients with Systemic Lupus Erythematosus (SLE) (n = 24), Systemic Sclerosis (SSc) (n = 24), Primary Raynauds Phenomenon (RP) (n = 17) and “other CTD” (n = 15) (Primary Sjogrens Syndrome, UCTD or MCTD) as well as 15 healthy controls were recruited. EMPs and PMPs were quantified using flow cytometry. Associations between MP levels and objective functional vascular assessments were evaluated.

Results

SLE patients had significantly higher EMPs compared with healthy controls and SSc patients. Higher PMP levels were noted in SSc and primary RP when compared to healthy controls and ‘other CTD’ patients. A modest correlation was noted between EMP and PMP levels in healthy controls (Spearman r = 0.6, p = 0.017). This relationship appeared stronger in SLE (r = 0.72, p < 0.0001) and other CTD patients (r = 0.75, p < 0.0001). The association between EMPs and PMPs was notably less strong in SSc (r = 0.45, p = 0.014) and RP (r = 0.37, p = 0.15). A significantly lower EMP/PMP ratio was detected in SSc/RP patients in comparison to both healthy controls and SLE/other CTD patients. Higher EMP and PMP levels were associated with higher digital perfusion following cold challenge in SSc. In contrast, higher PMP (but not EMP) levels were associated with lower digital perfusion at both baseline and following cold challenge in primary RP. Higher PMP levels were associated with greater endothelial-independent dilation in patients with SLE.

Conclusion

MP populations differ across the spectrum of AIRDS, possibly reflecting differences in vascular cell injury and activation. MP levels are associated with functional assessments of vascular function and might have a role as novel vascular biomarkers in AIRDs.

Significance and innovations

Levels of circulating endothelial and platelet microparticles differ between SSc/primary RP compared with SLE and other CTDs (UCTD, MCTD and Primary Sjogrens). MP release may occur within different vascular sites across these disease groups (macrovascular and microvascular).

The association between circulating MP levels and objective assessment of macro- and microvascular dysfunction within these disease areas suggests that MPs might have a useful

微颗粒(MPs)是来源于血管细胞和血管内细胞(如内皮细胞(EMPs)和血小板(pmp))的膜结合囊泡。我们研究了一系列自身免疫性风湿性疾病(AIRDs)的EMP和PMP数量,目的是比较EMP和PMP的水平及其之间的关系。方法招募系统性红斑狼疮(SLE) (n = 24)、系统性硬化症(SSc) (n = 24)、原发性雷氏现象(RP) (n = 17)和“其他CTD”(原发性Sjogrens综合征、UCTD或MCTD)患者以及15名健康对照组。流式细胞术定量测定EMPs和pmp。评估MP水平与客观血管功能评估之间的关系。结果SSc患者的emp明显高于健康对照组和SSc患者。与健康对照组和“其他CTD”患者相比,SSc和原发性RP患者的PMP水平较高。在健康对照组中,EMP和PMP水平之间存在适度的相关性(Spearman r = 0.6, p = 0.017)。这种关系在SLE中更为明显(r = 0.72, p <0.0001)和其他CTD患者(r = 0.75, p <0.0001)。在SSc (r = 0.45, p = 0.014)和RP (r = 0.37, p = 0.15)中,EMPs和pmp之间的相关性较弱。与健康对照组和SLE/其他CTD患者相比,SSc/RP患者的EMP/PMP比值显著降低。较高的EMP和PMP水平与SSc冷激后较高的数字灌注相关。相比之下,在原发性RP的基线和冷刺激后,较高的PMP(而不是EMP)水平与较低的数字灌注相关。在SLE患者中,较高的PMP水平与更大的内皮非依赖性扩张相关。结论mp群体在AIRDS谱上存在差异,可能反映了血管细胞损伤和激活的差异。MP水平与血管功能评估相关,可能在aird中作为新的血管生物标志物。与SLE和其他CTDs (UCTD、MCTD和原发性Sjogrens)相比,SSc/原发性RP的循环内皮细胞和血小板微粒水平存在差异。MP释放可能发生在这些疾病组(大血管和微血管)的不同血管部位。循环MP水平与这些疾病区域内大血管和微血管功能障碍的客观评估之间的关联表明,MPs可能作为CTDs内血管疾病的新型循环生物标志物具有有用的作用。
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引用次数: 28
Hemophagocytic lymphohistiocytosis in adults: An under recognized entity 成人的噬血细胞淋巴组织细胞病:一个未被认识的实体
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2016.12.002
Abdul Rashid Shah , Tariq Muzzafar , Rita Assi , Dawid Schellingerhout , Zeev Estrov , Gevorg Tamamyan , Hagop Kantarjian , Naval Daver

Hemophagocytic lymphohistiocytosis (HLH) is a syndrome of severe immune activation with macrophage and T-cell infiltration resulting in, multi organ damage. HLH may be primary or secondary in etiology. A high index of suspicion is essential for early diagnosis and treatment. Diagnostic criteria need to be refined and newer treatment options to be explored in order to improve survival especially in adult HLH and malignancy-associated HLH (M-HLH).

We report a case of malignancy associated HLH (M-HLH) in adult treated on one of the only FDA-approved protocols for adult HLH to highlight the diagnostic and therapeutic challenges of this disease entity.

噬血细胞性淋巴组织细胞增多症(HLH)是一种严重的免疫激活综合征,巨噬细胞和t细胞浸润导致多器官损伤。HLH的病因可为原发性或继发性。高度的怀疑指数对于早期诊断和治疗至关重要。诊断标准需要改进,新的治疗方案需要探索,以提高生存率,特别是在成人HLH和恶性肿瘤相关的HLH (M-HLH)。我们报告一例恶性相关HLH (M-HLH)的成人病例,该病例采用fda批准的唯一成人HLH治疗方案之一,以突出该疾病实体的诊断和治疗挑战。
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引用次数: 13
Understanding breast cancer – The long and winding road 了解乳腺癌-漫长而曲折的道路
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2017.01.001
Kiven Erique Lukong

Background

Despite a remarkable increase in the depth of our understanding and management of breast cancer in the past 50 years, the disease is still a major public health problem worldwide and poses significant challenges. The palpability of breast tumors has facilitated diagnosis and documentation since ancient times. The earliest descriptions of breast cancer date back to around 3500 BCE. For centuries to follow, theories by Hippocrates (460 BCE) and Galen (200 CE), attributing the cause of breast cancer to an “excess of black bile” and treatment options including the use of opium and castor oil, prevailed. Surgical resection was introduced in the 18th century. The advent of modern medicine led to the development of novel treatment options that include hormonal, targeted and chemo-therapies. There are still several therapeutic challenges including the treatment of triple negative breast cancer (TNBC), and overcoming drug resistance.

Scope of review

The increased incidence and awareness of breast cancer has led to significant changes in diagnosis and treatment in recent decades. But, mankind has come a long way. Herein, I have traced how our understanding of breast cancer has evolved from the early description of the disease around 460 BCE as “black bile-containing crab-like tumors” to the conventional as a heterogeneous disease with high degree of diversity between and within tumors, as well as among breast cancer patients. How is breast cancer treated today and how do risk factors, breast cancer subtype and drug resistance contribute to the therapeutic challenges at the turn of the 21st century?

Major conclusions

Breast cancer remains a serious public health issue worldwide. However, appreciable growth in our understanding of breast cancer in the past century has led to remarkable progress in the early detection, treatment and prevention of the disease. The clinical focus is shifting more towards tailored therapy as more targets are characterized and novel highly innovative approaches are developed.

General significance

Tracing the history of breast cancer, highlights how increased awareness of the disease, and progress in research and development have enhance our understanding of the disease.

尽管在过去的50年里,我们对乳腺癌的理解和管理有了显著的提高,但该疾病仍然是世界范围内的一个主要公共卫生问题,并构成了重大挑战。乳腺肿瘤的可触性自古以来就为诊断和记录提供了便利。关于乳腺癌的最早描述可以追溯到公元前3500年左右。在接下来的几个世纪里,希波克拉底(Hippocrates,公元前460年)和盖伦(Galen,公元200年)的理论将乳腺癌的病因归结为“黑胆汁过多”,治疗方法包括使用鸦片和蓖麻油。手术切除在18世纪被引入。现代医学的出现导致了新的治疗选择的发展,包括激素治疗,靶向治疗和化疗。目前仍存在一些治疗挑战,包括治疗三阴性乳腺癌(TNBC)和克服耐药性。近几十年来,乳腺癌发病率的提高和对乳腺癌认识的提高导致了乳腺癌诊断和治疗的重大变化。但是,人类已经取得了长足的进步。在这里,我追溯了我们对乳腺癌的认识是如何从公元前460年左右的早期描述为“含有黑胆汁的螃蟹样肿瘤”发展到传统的肿瘤之间和肿瘤内部以及乳腺癌患者之间高度多样性的异质性疾病。今天乳腺癌是如何治疗的?风险因素、乳腺癌亚型和耐药性是如何对21世纪初的治疗挑战做出贡献的?主要结论乳腺癌仍然是世界范围内一个严重的公共卫生问题。然而,在过去的一个世纪里,我们对乳腺癌的认识有了明显的增长,导致在早期发现、治疗和预防该疾病方面取得了显著进展。随着更多靶点的特征和新颖的高度创新的方法的开发,临床重点正在更多地转向量身定制的治疗。一般意义追溯乳腺癌的历史,强调如何提高对该疾病的认识,以及研究和开发的进展如何增强了我们对该疾病的了解。
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引用次数: 163
Pathogenicity in POLG syndromes: DNA polymerase gamma pathogenicity prediction server and database POLG综合征的致病性:DNA聚合酶γ致病性预测服务器和数据库
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2017.04.001
Anssi Nurminen , Gregory A. Farnum , Laurie S. Kaguni

DNA polymerase gamma (POLG) is the replicative polymerase responsible for maintaining mitochondrial DNA (mtDNA). Disorders related to its functionality are a major cause of mitochondrial disease. The clinical spectrum of POLG syndromes includes Alpers-Huttenlocher syndrome (AHS), childhood myocerebrohepatopathy spectrum (MCHS), myoclonic epilepsy myopathy sensory ataxia (MEMSA), the ataxia neuropathy spectrum (ANS) and progressive external ophthalmoplegia (PEO). We have collected all publicly available POLG-related patient data and analyzed it using our pathogenic clustering model to provide a new research and clinical tool in the form of an online server. The server evaluates the pathogenicity of both previously reported and novel mutations. There are currently 176 unique point mutations reported and found in mitochondrial patients in the gene encoding the catalytic subunit of POLG, POLG. The mutations are distributed nearly uniformly along the length of the primary amino acid sequence of the gene. Our analysis shows that most of the mutations are recessive, and that the reported dominant mutations cluster within the polymerase active site in the tertiary structure of the POLG enzyme. The POLG Pathogenicity Prediction Server (http://polg.bmb.msu.edu) is targeted at clinicians and scientists studying POLG disorders, and aims to provide the most current available information regarding the pathogenicity of POLG mutations.

DNA聚合酶(POLG)是负责维持线粒体DNA (mtDNA)的复制聚合酶。与其功能相关的疾病是线粒体疾病的主要原因。POLG综合征的临床谱包括alpers - hutenlocher综合征(AHS)、儿童心肌病谱(MCHS)、肌阵挛性癫痫肌病感觉性共济失调(MEMSA)、共济失调神经病变谱(ANS)和进行性外眼麻痹(PEO)。我们收集了所有公开可用的polg相关患者数据,并使用我们的致病聚类模型进行分析,以在线服务器的形式提供新的研究和临床工具。该服务器评估以前报告的和新突变的致病性。目前在线粒体患者中报道和发现的编码POLG催化亚基的基因中有176个独特的点突变。突变沿基因一级氨基酸序列的长度几乎均匀分布。我们的分析表明,大多数突变是隐性的,而报道的显性突变集中在POLG酶三级结构的聚合酶活性位点。POLG致病性预测服务器(http://polg.bmb.msu.edu)针对研究POLG疾病的临床医生和科学家,旨在提供有关POLG突变致病性的最新可用信息。
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引用次数: 33
Metabolomic analysis identifies differentially produced oral metabolites, including the oncometabolite 2-hydroxyglutarate, in patients with head and neck squamous cell carcinoma 代谢组学分析确定头颈部鳞状细胞癌患者口服代谢物的差异,包括肿瘤代谢物2-羟戊二酸
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2016.12.001
Pranab K. Mukherjee , Pauline Funchain , Mauricio Retuerto , Richard J. Jurevic , Nicole Fowler , Brian Burkey , Charis Eng , Mahmoud A Ghannoum

Background

Metabolomics represents a promising approach for discovering novel targets and biomarkers in head and neck squamous cell carcinoma (HNSCC). Here we used metabolomics to identify oral metabolites associated with HNSCC.

Methods

Tumor and adjacent normal tissue from surgical resections and presurgical oral washes as well as oral washes were collected from healthy participants. Metabolites extractions of these samples were analyzed by liquid chromatography-mass spectroscopy (LC/MS), LC/MS/MS and gas chromatography-MS (GC/MS).

Results

Among 28 samples obtained from 7 HNSCC cases and 7 controls, 422 metabolites were detected (269 identified and 153 unidentified). Oral washes contained 12 and 23 metabolites in healthy controls and HNSCC patients, respectively, with phosphate and lactate being the most abundant. Small molecules related to energy metabolism were significantly elevated in HNSCC patients compared to controls. Levels of beta-alanine, alpha-hydroxyisovalerate, tryptophan, and hexanoylcarnitine were elevated in HNSCC oral washes compared to healthy controls (range 7.8-12.2-fold). Resection tissues contained 22 metabolites, of which eight were overproduced in tumor by 1.9- to 12-fold compared to controls. TCA cycle analogs 2-hydroxyglutarate (2-HG) and 3-GMP were detected exclusively in tumor tissues. Targeted quantification of 2-HG in a representative HNSCC patient showed increase in tumor tissue (14.7 μg/mL), but undetectable in normal tissue. Moreover, high levels of 2-HG were detected in HNSCC cell lines but not in healthy primary oral keratinocyte cultures.

Conclusions

Oral metabolites related to energy metabolism were elevated in HNSCC, and acylcarnitine and 2HG may have potential as non-invasive biomarkers. Further validation in clinical studies is warranted.

代谢组学是发现头颈部鳞状细胞癌(HNSCC)新靶点和生物标志物的一种很有前途的方法。在这里,我们使用代谢组学来鉴定与HNSCC相关的口服代谢物。方法收集健康受试者手术切除及术前口腔洗液及口腔洗液的肿瘤及邻近正常组织。采用液相色谱-质谱(LC/MS)、液相色谱-质谱(LC/MS /MS)和气相色谱-质谱(GC/MS)对样品的代谢物提取进行分析。结果在7例HNSCC病例和7例对照的28份样本中,检出422种代谢物,其中鉴定的269种,未鉴定的153种。口腔洗液在健康对照组和恶性鳞癌患者中分别含有12种和23种代谢物,其中磷酸盐和乳酸含量最高。与对照组相比,HNSCC患者中与能量代谢相关的小分子显著升高。与健康对照组相比,HNSCC口腔洗液中β -丙氨酸、α -羟基异戊酸酯、色氨酸和己醇基肉碱的水平升高(范围为7.8-12.2倍)。切除组织中含有22种代谢物,其中8种代谢物在肿瘤中过量产生,是对照组的1.9- 12倍。TCA循环类似物2-羟基戊二酸(2-HG)和3-GMP仅在肿瘤组织中检测到。代表性HNSCC患者2-HG靶向定量显示,肿瘤组织中2-HG升高(14.7 μg/mL),正常组织中未检测到。此外,在HNSCC细胞系中检测到高水平的2-HG,而在健康的原代口腔角化细胞培养中未检测到。结论与能量代谢相关的al代谢产物在HNSCC中升高,酰基肉碱和2HG可能具有作为无创生物标志物的潜力。在临床研究中进一步验证是有必要的。
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引用次数: 23
The plasma lipidome in acute myeloid leukemia at diagnosis in relation to clinical disease features 急性髓系白血病诊断时血浆脂质组与临床疾病特征的关系
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2017.03.002
Thomas Pabst , Linda Kortz , Georg M. Fiedler , Uta Ceglarek , Jeffrey R. Idle , Diren Beyoğlu

Background

Early studies established that certain lipids were lower in acute myeloid leukemia (AML) cells than normal leukocytes. Because lipids are now known to play an important role in cell signaling and regulation of homeostasis, and are often perturbed in malignancies, we undertook a comprehensive lipidomic survey of plasma from AML patients at time of diagnosis and also healthy blood donors.

Methods

Plasma lipid profiles were measured using three mass spectrometry platforms in 20 AML patients and 20 healthy blood donors. Data were collected on total cholesterol and fatty acids, fatty acid amides, glycerolipids, phospholipids, sphingolipids, cholesterol esters, coenzyme Q10 and eicosanoids.

Results

We observed a depletion of plasma total fatty acids and cholesterol, but an increase in certain free fatty acids with the observed decline in sphingolipids, phosphocholines, triglycerides and cholesterol esters probably driven by enhanced fatty acid oxidation in AML cells. Arachidonic acid and precursors were elevated in AML, particularly in patients with high bone marrow (BM) or peripheral blasts and unfavorable prognostic risk. PGF2α was also elevated, in patients with low BM or peripheral blasts and with a favorable prognostic risk. A broad panoply of lipid classes is altered in AML plasma, pointing to disturbances of several lipid metabolic interconversions, in particular in relation to blast cell counts and prognostic risk.

Conclusions

These data indicate potential roles played by lipids in AML heterogeneity and disease outcome.

General significance

Enhanced catabolism of several lipid classes increases prognostic risk while plasma PGF2α may be a marker for reduced prognostic risk in AML.

研究表明,急性髓性白血病(AML)细胞中的某些脂质比正常白细胞低。由于现在已知脂质在细胞信号传导和体内平衡调节中起重要作用,并且在恶性肿瘤中经常受到干扰,我们对诊断时AML患者和健康献血者的血浆进行了全面的脂质组学调查。方法采用3种质谱分析平台对20例急性髓系白血病患者和20例健康献血者的血浆脂质谱进行测定。收集总胆固醇、脂肪酸、脂肪酸酰胺、甘油脂、磷脂、鞘脂、胆固醇酯、辅酶Q10和二十烷类化合物的数据。结果:我们观察到血浆总脂肪酸和胆固醇的消耗,但某些游离脂肪酸的增加,观察到鞘脂、磷脂、甘油三酯和胆固醇酯的下降,可能是由AML细胞中脂肪酸氧化增强引起的。花生四烯酸和前体在AML中升高,特别是在骨髓(BM)或外周细胞高且预后风险不利的患者中。在低BM或外周细胞患者中,PGF2α也升高,预后风险良好。AML血浆中广泛的脂质类别发生改变,指出几种脂质代谢相互转换的紊乱,特别是与母细胞计数和预后风险有关。结论这些数据表明脂质在AML异质性和疾病结局中发挥潜在作用。几种脂类分解代谢增强可增加预后风险,而血浆PGF2α可能是AML预后风险降低的标志。
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引用次数: 38
A novel dominant D109A CRYAB mutation in a family with myofibrillar myopathy affects αB-crystallin structure 肌原纤维性肌病家族中一种新的显性D109A CRYAB突变影响α b -晶体蛋白结构
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2016.11.004
Jakub P. Fichna , Anna Potulska-Chromik , Przemysław Miszta , Maria Jolanta Redowicz , Anna M. Kaminska , Cezary Zekanowski , Sławomir Filipek

Myofibrillar myopathy (MFM) is a group of inherited muscular disorders characterized by myofibrils dissolution and abnormal accumulation of degradation products. So far causative mutations have been identified in nine genes encoding Z-disk proteins, including αB-crystallin (CRYAB), a small heat shock protein (also called HSPB5).

Here, we report a case study of a 63-year-old Polish female with a progressive lower limb weakness and muscle biopsy suggesting a myofibrillar myopathy, and extra-muscular multisystemic involvement, including cataract and cardiomiopathy. Five members of the proband's family presented similar symptoms. Whole exome sequencing followed by bioinformatic analysis revealed a novel D109A mutation in CRYAB associated with the disease.

Molecular modeling in accordance with muscle biopsy microscopic analyses predicted that D109A mutation influence both structure and function of CRYAB due to decreased stability of oligomers leading to aggregate formation. In consequence disrupted sarcomere cytoskeleton organization might lead to muscle pathology. We also suggest that mutated RQDE sequence of CRYAB could impair CRYAB chaperone-like activity and promote aggregation of lens crystallins.

肌原纤维肌病(MFM)是一组以肌原纤维溶解和降解产物异常积累为特征的遗传性肌肉疾病。到目前为止,已经在编码z盘蛋白的9个基因中发现了致病突变,包括α b -晶体蛋白(CRYAB),一种小型热休克蛋白(也称为HSPB5)。在这里,我们报告一个63岁波兰女性的病例研究,其进行性下肢无力和肌肉活检提示肌纤维性肌病,肌肉外多系统累及,包括白内障和心肌病。先证者的五名家庭成员也出现了类似的症状。全外显子组测序和生物信息学分析显示,CRYAB中存在与该疾病相关的新型D109A突变。根据肌肉活检显微分析的分子模型预测,D109A突变会影响CRYAB的结构和功能,因为低聚物的稳定性降低,导致聚集形成。因此,肌节细胞骨架组织的破坏可能导致肌肉病理。我们还发现CRYAB的RQDE序列突变会损害CRYAB的伴侣蛋白样活性,促进晶状体结晶蛋白的聚集。
{"title":"A novel dominant D109A CRYAB mutation in a family with myofibrillar myopathy affects αB-crystallin structure","authors":"Jakub P. Fichna ,&nbsp;Anna Potulska-Chromik ,&nbsp;Przemysław Miszta ,&nbsp;Maria Jolanta Redowicz ,&nbsp;Anna M. Kaminska ,&nbsp;Cezary Zekanowski ,&nbsp;Sławomir Filipek","doi":"10.1016/j.bbacli.2016.11.004","DOIUrl":"10.1016/j.bbacli.2016.11.004","url":null,"abstract":"<div><p>Myofibrillar myopathy (MFM) is a group of inherited muscular disorders characterized by myofibrils dissolution and abnormal accumulation of degradation products. So far causative mutations have been identified in nine genes encoding Z-disk proteins, including αB-crystallin (CRYAB), a small heat shock protein (also called HSPB5).</p><p>Here, we report a case study of a 63-year-old Polish female with a progressive lower limb weakness and muscle biopsy suggesting a myofibrillar myopathy, and extra-muscular multisystemic involvement, including cataract and cardiomiopathy. Five members of the proband's family presented similar symptoms. Whole exome sequencing followed by bioinformatic analysis revealed a novel D109A mutation in <em>CRYAB</em> associated with the disease.</p><p>Molecular modeling in accordance with muscle biopsy microscopic analyses predicted that D109A mutation influence both structure and function of CRYAB due to decreased stability of oligomers leading to aggregate formation. In consequence disrupted sarcomere cytoskeleton organization might lead to muscle pathology. We also suggest that mutated RQDE sequence of CRYAB could impair CRYAB chaperone-like activity and promote aggregation of lens crystallins.</p></div>","PeriodicalId":72344,"journal":{"name":"BBA clinical","volume":null,"pages":null},"PeriodicalIF":0.0,"publicationDate":"2017-06-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://sci-hub-pdf.com/10.1016/j.bbacli.2016.11.004","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"54181930","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"OA","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
引用次数: 35
Proteomic analysis of bronchoalveolar lavage fluid (BALF) from lung cancer patients using label-free mass spectrometry 肺癌患者支气管肺泡灌洗液(BALF)的蛋白质组学分析
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2017.03.001
Abduladim Hmmier , Michael Emmet O'Brien , Vincent Lynch , Martin Clynes , Ross Morgan , Paul Dowling

Background

Lung cancer is the leading cause of cancer-related mortality in both men and women throughout the world. The need to detect lung cancer at an early, potentially curable stage, is essential and may reduce mortality by 20%. The aim of this study was to identify distinct proteomic profiles in bronchoalveolar fluid (BALF) and plasma that are able to discriminate individuals with benign disease from those with non-small cell lung cancer (NSCLC).

Methods

Using label-free mass spectrometry analysis of BALF during discovery-phase analysis, a significant number of proteins were found to have different abundance levels when comparing control to adenocarcinoma (AD) or squamous cell lung carcinoma (SqCC). Validation of candidate biomarkers identified in BALF was performed in a larger cohort of plasma samples by detection with enzyme-linked immunoassay.

Results

Four proteins (Cystatin-C, TIMP-1, Lipocalin-2 and HSP70/HSPA1A) were selected as a representative group from discovery phase mass spectrometry BALF analysis. Plasma levels of TIMP-1, Lipocalin-2 and Cystatin-C were found to be significantly elevated in AD and SqCC compared to control.

Conclusion

The results presented in this study indicate that BALF is an important proximal biofluid for the discovery and identification of candidate lung cancer biomarkers.

General significance

There is good correlation between the trend of protein abundance levels in BALF and that of plasma which validates this approach to develop a blood biomarker to aid lung cancer diagnosis, particularly in the era of lung cancer screening. The protein signatures identified also provide insight into the molecular mechanisms associated with lung malignancy.

背景肺癌是全世界男性和女性癌症相关死亡的主要原因。在可能治愈的早期阶段发现肺癌是至关重要的,这可能会使死亡率降低20%。本研究的目的是鉴定支气管肺泡液(BALF)和血浆中能够区分良性疾病个体与非小细胞肺癌(NSCLC)个体的不同蛋白质组学特征。方法在发现阶段对BALF进行无标记质谱分析,与腺癌(AD)或鳞状细胞肺癌(SqCC)相比,发现大量蛋白质具有不同的丰度水平。通过酶联免疫分析法检测,在更大的血浆样本队列中验证了在BALF中鉴定的候选生物标志物。结果4个蛋白(Cystatin-C、TIMP-1、Lipocalin-2和HSP70/HSPA1A)作为发现期质谱BALF分析的代表性组。与对照组相比,AD和SqCC患者血浆中TIMP-1、Lipocalin-2和Cystatin-C水平显著升高。结论BALF是发现和鉴定肺癌候选生物标志物的重要近端生物液。BALF中蛋白质丰度水平的趋势与血浆中蛋白质丰度水平的趋势之间存在良好的相关性,这证实了开发血液生物标志物来帮助肺癌诊断的方法,特别是在肺癌筛查时代。鉴定的蛋白质特征也提供了与肺恶性肿瘤相关的分子机制的见解。
{"title":"Proteomic analysis of bronchoalveolar lavage fluid (BALF) from lung cancer patients using label-free mass spectrometry","authors":"Abduladim Hmmier ,&nbsp;Michael Emmet O'Brien ,&nbsp;Vincent Lynch ,&nbsp;Martin Clynes ,&nbsp;Ross Morgan ,&nbsp;Paul Dowling","doi":"10.1016/j.bbacli.2017.03.001","DOIUrl":"10.1016/j.bbacli.2017.03.001","url":null,"abstract":"<div><h3>Background</h3><p>Lung cancer is the leading cause of cancer-related mortality in both men and women throughout the world. The need to detect lung cancer at an early, potentially curable stage, is essential and may reduce mortality by 20%. The aim of this study was to identify distinct proteomic profiles in bronchoalveolar fluid (BALF) and plasma that are able to discriminate individuals with benign disease from those with non-small cell lung cancer (NSCLC).</p></div><div><h3>Methods</h3><p>Using label-free mass spectrometry analysis of BALF during discovery-phase analysis, a significant number of proteins were found to have different abundance levels when comparing control to adenocarcinoma (AD) or squamous cell lung carcinoma (SqCC). Validation of candidate biomarkers identified in BALF was performed in a larger cohort of plasma samples by detection with enzyme-linked immunoassay.</p></div><div><h3>Results</h3><p>Four proteins (Cystatin-C, TIMP-1, Lipocalin-2 and HSP70/HSPA1A) were selected as a representative group from discovery phase mass spectrometry BALF analysis. Plasma levels of TIMP-1, Lipocalin-2 and Cystatin-C were found to be significantly elevated in AD and SqCC compared to control.</p></div><div><h3>Conclusion</h3><p>The results presented in this study indicate that BALF is an important proximal biofluid for the discovery and identification of candidate lung cancer biomarkers.</p></div><div><h3>General significance</h3><p>There is good correlation between the trend of protein abundance levels in BALF and that of plasma which validates this approach to develop a blood biomarker to aid lung cancer diagnosis, particularly in the era of lung cancer screening. The protein signatures identified also provide insight into the molecular mechanisms associated with lung malignancy.</p></div>","PeriodicalId":72344,"journal":{"name":"BBA clinical","volume":null,"pages":null},"PeriodicalIF":0.0,"publicationDate":"2017-06-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://sci-hub-pdf.com/10.1016/j.bbacli.2017.03.001","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"34845864","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"OA","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
引用次数: 26
A post-publication analysis of the idealized upper reference value of 2.5 mIU/L for TSH: Time to support the thyroid axis with magnesium and iron especially in the setting of reproduction medicine TSH理想上参考值2.5 mIU/L的发表后分析:用镁和铁支持甲状腺轴的时间,特别是在生殖医学的背景下
BBA clinical
Pub Date : 2017-06-01 DOI: 10.1016/j.bbacli.2017.03.003
Roy Moncayo, Helga Moncayo

Laboratory medicine approaches the evaluation of thyroid function mostly through the single determination of the blood level of thyroid stimulating hormone (TSH). Some authors have suggested an upper reference value for TSH of 2.5 mIU/L. This suggestion has not been confirmed by recent clinical studies. These studies have delivered a clinically valid reference range going from 0.3 to 3.5 mIU/L. These values are valid for both for the general population as well as in the setting of fertility and pregnancy.

Current biochemical evidence about the elements required to maintain thyroid function shows that these not only include dietary iodine but also magnesium, iron, selenium and coenzyme Q10. Iron is important for the synthesis of thyroid peroxidase; magnesium-ATP contributes to the active process of iodine uptake; iodine has to be sufficiently present in the diet; selenium acts through selenoproteins to protect the thyroid cell during hormone synthesis and in deiodination of thyroxine; coenzyme Q10 influences thyroid vascularity. As a consequence, good clinical practice requires additional biochemical information on the blood levels of magnesium, selenium, coenzyme Q10 as well as iron status.

Since these elements are also important for the maintenance of reproductive function, we postulate that they constitute the connecting link between both endocrine systems.

检验医学对甲状腺功能的评价大多是通过血液中促甲状腺激素(TSH)水平的单一测定。一些作者建议TSH的最高参考值为2.5 mIU/L。这一建议尚未得到近期临床研究的证实。这些研究提供了0.3 - 3.5 mIU/L的临床有效参考范围。这些值既适用于一般人群,也适用于生育和怀孕情况。目前关于维持甲状腺功能所需元素的生化证据表明,这些元素不仅包括膳食碘,还包括镁、铁、硒和辅酶Q10。铁对甲状腺过氧化物酶的合成很重要;镁- atp参与碘吸收的活性过程;饮食中必须有足够的碘;硒通过硒蛋白在激素合成和甲状腺素脱碘过程中保护甲状腺细胞;辅酶Q10影响甲状腺血管。因此,良好的临床实践需要额外的血液中镁、硒、辅酶Q10和铁的生化信息。由于这些元素对维持生殖功能也很重要,我们假设它们构成了两个内分泌系统之间的连接纽带。
{"title":"A post-publication analysis of the idealized upper reference value of 2.5 mIU/L for TSH: Time to support the thyroid axis with magnesium and iron especially in the setting of reproduction medicine","authors":"Roy Moncayo,&nbsp;Helga Moncayo","doi":"10.1016/j.bbacli.2017.03.003","DOIUrl":"10.1016/j.bbacli.2017.03.003","url":null,"abstract":"<div><p>Laboratory medicine approaches the evaluation of thyroid function mostly through the single determination of the blood level of thyroid stimulating hormone (TSH). Some authors have suggested an upper reference value for TSH of 2.5<!--> <!-->mIU/L. This suggestion has not been confirmed by recent clinical studies. These studies have delivered a clinically valid reference range going from 0.3 to 3.5<!--> <!-->mIU/L. These values are valid for both for the general population as well as in the setting of fertility and pregnancy.</p><p>Current biochemical evidence about the elements required to maintain thyroid function shows that these not only include dietary iodine but also magnesium, iron, selenium and coenzyme Q10. Iron is important for the synthesis of thyroid peroxidase; magnesium-ATP contributes to the active process of iodine uptake; iodine has to be sufficiently present in the diet; selenium acts through selenoproteins to protect the thyroid cell during hormone synthesis and in deiodination of thyroxine; coenzyme Q10 influences thyroid vascularity. As a consequence, good clinical practice requires additional biochemical information on the blood levels of magnesium, selenium, coenzyme Q10 as well as iron status.</p><p>Since these elements are also important for the maintenance of reproductive function, we postulate that they constitute the connecting link between both endocrine systems.</p></div>","PeriodicalId":72344,"journal":{"name":"BBA clinical","volume":null,"pages":null},"PeriodicalIF":0.0,"publicationDate":"2017-06-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://sci-hub-pdf.com/10.1016/j.bbacli.2017.03.003","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"34913538","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"OA","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
引用次数: 33
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