网织红细胞参数对遗传性球形红细胞增多症筛查价值

目的 探讨各红细胞和网织红细胞参数对遗传性球形红细胞增多症（HS）的筛查诊断价值。方法 收集本院2010年1月—2021年12月确诊的HS患者41例,设为HS组,同时收集40例自身免疫性溶血性贫血（AIHA)患者设为AIHA组,50例地中海贫血（THAL）患者设为THAL组,另选取50例健康体检者为正常对照组。运用t检验比较各组各血细胞参数之间的差异,并采用受试者工作特征（ROC）曲线分析各红细胞参数和网织红细胞参数对HS的筛查诊断价值。结果 HS组平均红细胞体积（MCV）、平均网织红细胞体积（MRV）、平均球形红细胞体积（MSCV）明显低于AIHA组,而平均血红蛋白浓度（MCHC）则明显高于AIHA组（均P<0.05）。HS组MCV、MRV、MSCV均低于正常对照组,MCHC、Ret百分率则明显高于正常对照组,差异有统计学意义（均P＜0.05）。HS组和THAL组比较,除Hb外,其余参数差异均有统计学意义（P＜0.05）。HS组MSCV低于MCV,而THAL组MSCV高于MCV。HS组MSCV-MCV与其他3组比较差异均有统计学意义（P＜0.05）。ROC曲线分析发现MCHC诊断HS的最佳截断值为338.5 g/L,其灵敏度、特异性分别为94.6%和73.7%;MRV最佳截断值为97.1 fL,其灵敏度为91.9%,特异性为86.9%,MSCV-MCV最佳截断值为-3.4 fL,其灵敏度、特异性为94.6%、89.4%。MRV联合MCHC、MRV联合MSCV-MCV ROC曲线下面积（AUC）分别为0.978、0.988,均大于MCHC、MRV、MSCV-MCV任一指标的AUC。结论 MCHC、MRV、MSCV、MSCV-MCV等指标对于HS的鉴别诊断具有重要的参考价值。MCHC不是筛查诊断HS的理想指标,MRV和MSCV-MCV具有较高的预测价值,而联合指标筛查诊断价值要优于单一指标     

Prevalence of hereditary ataxias and spastic paraplegias in Molise,a region of Italy

Summary An epidemiological survey of hereditary ataxias and paraplegias was conducted in Molise, a region of Italy (335, 211 inhabitants on 1 January 1989). Total prevalence was 7.5 x 10^–5 inhabitants (95% confidence limits 4.8–11.1). There were 7 patients with Friedreich's disease, 5 with early onset cerebellar ataxia with retained tendon reflexes, 4 with ataxia-telangiectasia, 9 with hereditary spastic paraplegias (2 autosomal dominant and 7 autosomal recessive cases). There was no patient with autosomal dominant cerebellar ataxia.     

FG syndrome in a premature male

A 30-week premature male infant is presented with dolichocephaly, frontal bossing, down-slanting palpebral fissures, hypertelorism, long philtrum, micrognathia, cleft palate, and imperforate anus. He is the fifth patient to be presented with FG syndrome and sensorineural deafness. The patient's syndromic manifestations became more obvious during an inpatient observation period of 3 months.     

装潢居室空气中挥发性化学物的遗传毒性研究

目的探讨装潢居室空气中挥发性化合物的遗传毒性.方法采用小鼠骨髓嗜多染性红细胞微核试验和小鼠精子畸形试验检测居室装潢后空气中挥发性化合物的遗传毒性.结果该化合物对小鼠呼吸系统有明显的刺激作用,与阴性对照组比较,高、中、低剂量组的微核率、精子畸形率均有显著差异性.结论居室装潢后室内空气中挥发性化合物具有遗传毒性作用.     

鄂西苗族氨基糖甙类抗生素致聋患者的mtDNA1555位点突变研究

目的为探讨遗传因素在鄂西苗族氨基糖甙类抗生素致聋(AAID)发生中的作用,从分子水平研究该病的发病机制.方法对鄂西苗族部分家系及医学散发病例通过问卷调查和进行听力测试,确诊为AAID的82名患者,采外周血作PCR-RFLP分析,对照组为正常苗族50名.结果82名患者中27例具有mtDNA1555A→G异质性突变,10例为均质性突变,该位点突变率为45.1%,其中异质性突变占72,9%,而对照组均无此突变.结论mtDNA1555A→G突变是鄂西苗族个体对氨基糖甙类抗生素易感致聋的分子基础,异质性突变在苗族AAID中发生率较高.     

Hepatic Function and Fibrinolysis in Patients with Hereditary Angioedema Undergoing Long-Term Treatment with Tranexamic Acid

Prophylactic treatment with antifibrinolytic agents, epsilon-aminocapriod and tranexamic acid, reduces the incidence and severits of attacks in patients with hereditary angioedema. Long-term ellectivenessor risk of antifibrinolytic agents has not been established. Sixteen patients needing continuous prophylaxis because of frequency and severity of attacks were treated with tranexamic acid. In four patients this treatment was ineffective and the drug was withdrawn after 2 months. A remission or reduction in the frequency or serverity of attacks was observed in 12 patients treated for a period ranging from 8 to 34 months. Hepatic tests and blood fibrinolytic activity were not influenced by long term oral treatment with tranexamic acid.     

Micropuncture studies on the influence of antidiuretic hormone on tubular fluid reabsorption in rats with hereditary hypothalamic diabetes insipidus

Summary Micropuncture studies were carried out on rats with hereditary hypothalamic diabetes insipidus, in order to measure net sodium and water reabsorption in proximal convolutions and short loops of Henle during water diuresis and ADH-induced antidiuresis. Intravenous infusion of 0.15 mU ADH per minute reduced urine flow from 74.5 l per kidney per minute to 10.8 l, and increased urine osmolality from 117 to 605 mOsm/kg. These changes could be reversed by stopping ADH.ADH did not alter the fractional reabsorption of fluid or the reabsorptive capacity for sodium in the proximal tubules. Nor did it change glomerular filtration rates of single superficial nephrons or of the entire kidney.Fractional reabsorption of the glomerular filtrate up to the early distal convolution was significantly higher (82.0%) in water diuresis than in antidiuresis (74.4%). Since this reabsorption remained unchanged in the proximal convolutions, the decreased reabsorption during antidiuresis must have occurred in the short loops. Fractional reabsorption of sodium up to the early distal tubule was essentially identical during water diuresis and antidiuresis, indicating that ADH does not enhance urinary concentration by increasing the reabsorption of sodium from short loops.On leave of absence from the Department of Physiology, Dartmouth Medical School, Hannover, N. H., from January to June, 1967. Recipient of USPHS Research Career Program Award 5-K3-GM-21, 786.     

Neuroradiology and clinical aspects of Usher syndrome

We describe the neurological evaluation and MRI analysis of 30 patients, belonging to 16 families with Usher syndrome (US) type I and type II (US1 and US2). In addition to the classic visual and audiological abnormalities seen in these patients, we observed abnormal gait in 88.9% of US1 and in 66.7% of US2 patients and abnormal coordination in 33.4% of US1, and in 58.3% of US2. Borderline mental retardation, depression or bipolar affective disorder were observed in 16.7% of US1 and 33.3% of US2 patients. MRI analysis showed cerebellar abnormalities in 50% of US 1 and 75% of US2 patients, but no clear correlation was observed between structural abnormalities and clinical findings. A pattern for the MRI classification of US patients is suggested.     

Mutations in the gene encoding KIAA1199 protein,an inner-ear protein expressed in Deiters’ cells and the fibrocytes,as the cause of nonsyndromic hearing loss

We report three possibly disease-causing point mutations in one of the inner-ear-specific genes, KIAA1199. We identified an R187C mutation in one family, an R187H mutation in two unrelated families, and an H783Y mutation in one sporadic case of nonsyndromic hearing loss. In situ hybridization indicated that the murine homolog of KIAA1199 mRNA is expressed specifically in Deiters cells in the organ of Corti at postnatal day zero (Pn) P0 before the onset of hearing, but expression in those cells disappears by day P7. The signal of KIAA1199 was also observed in fibrocytes of the spiral ligament and the spiral limbus through to P21, when the murine cochlea matures. Thus, the gene product may be involved in uptake of potassium ions or trophic factors with a particular role in auditory development. Although the R187C and R187H mutations did not appear to affect subcellular localization of the gene product in vitro, the H783Y mutation did present an unusual cytoplasmic distribution pattern that could underlie the molecular mechanism of hearing impairment. Our data bring attention to a novel candidate for hearing loss and indicate that screening of mutations in inner-ear-specific genes is likely to be an efficient approach to finding genetic elements responsible for deafness.Nucleotide sequence data reported herein are available in the DDBJ/EMBL/GenBank databases; for details, see the electronic eatabase section of this article.