全染色体涂抹探针在女性罗伯逊易位携带者植入前遗传学诊断中的临床应用

目的应用全染色体涂抹探针（whole chromosome painting probe，WCP）对女性罗伯逊易位携带者进行卵母细胞第一极体的植入前遗传学诊断（preimplantation genetic diagnosis，PGD）。方法应用全染色体涂抹探针进行第一极体荧光原位杂交，对4例女方罗伯逊易位携带者进行了4个周期的PGD。患者染色体核型均为45，XX，der（13；14），（q10；q10）。所有周期取卵后6h内通过活检取出第一极体，采用WCP探针进行荧光原位杂交，受精后第3天选择染色体组成正常或平衡的胚胎进行宫腔内移植。结果4个周期共获卵61个，其中54个成熟可进行活检，活检成功率92．6％（50／54），固定成功率90．O％（45／50）。40个获得明确诊断，总体诊断率为74．1％（40／54）。卵胞浆内单精子注射后受精率64．8％（35／54），优质胚胎率为65．7％（23／35）。获得2例临床妊娠。其中1例于孕9周胚胎停止发育，绒毛染色体分析核型为45，X；另1例产前诊断证实核型为46，XX。2006年6月足月分娩一正常活女婴。结论全染色体涂抹探针可准确区分正常、平衡以及异常卵子，从而可有效应用于女性染色体易位携带者的PGD。     

运用全染色体探针FISH技术进行罗伯逊易位携带者胚胎植入前诊断

目的运用全染色体探针荧光原位杂交技术(fluorescent in situ hybridization ,FISH)对14/21罗伯逊易位携带者的胚胎进行植入前遗传学诊断,达到优生目的.方法应用FITC、Texas标记的21/14全染色体探针对14/21罗伯逊易位携带者的胚胎活检后的单个卵裂球进行遗传学检测,选择正常信号或携带者信号核型胚胎进行移植.结果常规单精子显微注射-胚胎移植(intracytoplasmic sperm injection,ICSI)后获取胚胎12个,活检优质胚胎11个,杂交后有信号胚胎7个,其中1个正常胚胎,1个携带者胚胎;1个14单体胚胎,1个21单体胚胎,1个21三体胚胎,另2个胚胎活检后均为21号二体,无14号信号.结论运用14/21全染色体探针荧光原位杂交技术对14/21罗伯逊易位携带者的胚胎进行植入前遗传学诊断是能够将正常核型胚胎挑选出来进行移植,从而达到优生目的.     

植入前诊断罗伯逊易位一例

目的　对 1例罗伯逊易位患者进行植入前胚胎遗传学诊断。方法　应用 Vysis L SI13q14 ,Tel Vysion14 q探针对卵裂球对进行荧光原位杂交分析。结果　荧光原位杂交结果显示 1个胚胎的染色体正常或为携带者 ;7个胚胎染色体异常 ,其中 1个 14三体 ,4个 14三体 13单体 ,2个 13三体 14单体 ;2个胚胎未见明确信号。移植 1个染色体正常或平衡易位的胚胎后 ,孕 10周复查 B超示胎儿发育良好。结论　罗伯逊易位的植入前胚胎遗传学诊断方法有效。     

一例罗伯逊易位携带者的胚胎植入前遗传学诊断

目的　探讨植入前遗传学诊断 (preimplantation genetic diagnosis,PGD)用于筛选罗伯逊易位携带者无遗传缺陷后代的可行性及风险。方法　 1对因男方携带易位 (13;14 )染色体并伴少、弱精的原发不孕夫妇 ,经激素超促排卵和单精子卵胞浆内注射 (intracytoplasmic sperm injection,ICSI)进行体外受精(in vitro fertilization,IVF) ,当胚胎发育到 6～ 8细胞阶段 (受精后第 3天 )时 ,用酸化法活检 ,从每个胚胎中取出单个分裂球 ,用 L SI 13q和 Tel 14 q探针进行荧光原位杂交 (fluorescence in situ hybridization,FISH)检测 ,继续培养活检后的胚胎到第 2天 ,并选择正常胚胎移植 ,获临床妊娠后 ,于妊娠中期行羊水细胞染色体检查。结果　活检 10个胚胎 ,获得 8个 FISH诊断结果 :5 0 % (4/8)正常或平衡的胚胎 ,37.5 % (3/8)不平衡的胚胎 ,12 .5 % (1/8)不确定。将诊断正常或平衡的胚胎 3枚于活检第 2天移植入母体宫腔 ,获临床单胎妊娠 ,产前诊断证实胎儿核型为 4 6 ,XY,完全正常 ,现分娩一正常男婴。结论　需行辅助生殖技术治疗的患者 ,当携带有罗伯逊易位时 ,PGD用于筛除异常胚胎 ,解决患者的生育障碍、预防严重遗传病胎儿的产生具有重要价值。     

临沂地区58例罗伯逊易位携带者的遗传学分析北大核心CSCD

目的探讨临沂地区各种罗伯逊易位携带者异常妊娠的几率,计算各种核型的比例,统计罗伯逊易位携带者和罗伯逊易位型21三体患者的性别比,为遗传咨询提供依据。方法采用外周血淋巴细胞培养技术制备染色体,通过G显带进行核型分析,对异常核型者进行家系调查和遗传学分析。结果在10339例进行遗传咨询的人群中,共检出58例罗伯逊易位携带者和22例罗伯逊易位型21三体患者,罗伯逊易位携带者中der（13;14）和der（14;21）所占比例分别为50．00％和17．24％;易位型21三体患者只有der（14;21）和der（21;21）两种核型,分别占54．55％和45．45％。罗伯逊易位携带者男女之比为0．57：1（21／37）,与正常人群差异极为显著（P〈0．05）;易位型21三体中男女之比为1．75：1（14／8）,与正常人群无显著差异（P〉0．05）。53例非同源罗伯逊易位携带者中有7例男性因精子质量极差不育,4例未到生育年龄,其余42例平均流产率为92．86％（39／42）,平均流产（或其他异常妊娠）2．26次（95／42）,非同源罗伯逊异位携带者异常妊娠和正常妊娠的比例为7．4：1（96／13）。夫妇一方为同源罗伯逊易位携带者的异常妊娠率为100％,平均异常妊娠2．8次。结论罗伯逊易位是造成反复流产及生育易位型21三体患儿的主要遗传学原因之一,不同核型的个体在临床表现上有很大的差异。针对不同核型的罗伯逊易位携带者在遗传咨询时应有所侧重。对这些患者进行染色体检查、遗传咨询和生育指导非常必要。     

紧密连锁的多态性位点在β地中海贫血植入前遗传学诊断中的应用

目的 探讨与β珠蛋白基因紧密连锁的多态性位点HumTH01在β地中海贫血（β地贫）植入前遗传学诊断（preimplantation genetic diagnosis，PGD）中的作用。方法 对4例已出生重型β地贫患儿的、双方均为β地贫基因携带者的夫妇进行了6个周期的PGD治疗，应用多重巢式PCR同时检测β珠蛋白基因及HumTH01基因，选择健康的胚胎移植入子宫。结果 6个周期共活检44个胚胎，获得44个卵裂球，其中41个卵裂球扩增成功，35个胚胎经PCR分析后获得明确诊断，移植了14个胚胎，获得1例临床妊娠。孕17周时经脐带血穿刺，证实为完全正常胚胎，现已出生一正常女婴。单个卵裂球平均扩增效率为89．7％，等位基因脱扣（allele drop-out，ADO）率为14．4％。HumTH01基因可以帮助检测出ADO及污染的发生。结论 本研究为国内首次报道应用多重巢式PCR同时检测β珠蛋白基因及HumTH01基因对β地贫进行植入前遗传学诊断并成功获得临床妊娠。在PGD中同时检测与β珠蛋白基因紧密连锁的多态性位点可以降低PGD中由于ADO及污染造成的误诊的风险。     

植入前诊断t(5;14)(q11;q23)相互易位一例

目的对一例相互易位携带者进行胚胎植入前诊断，研究商业化探针组合在相互易位植入前诊断中的应用价值。方法受精后第3天对4个卵裂球进行活检，采用二步荧光原位杂交技术检测卵裂球中2对易位染色体状态，共选用5号，14号染色体断裂点远侧的ERG1和Tel 14q,以及5号染色体断裂点近侧的D5S23 3个探针。结果4个细胞裂解后均呈现单个完整细胞核，二步荧光原位杂交中各细胞核均有清晰明亮的杂交信号，各胚胎ERG 1/D5S23/Tel 14q信号数分别为：1号胚胎3/2/1；2号胚胎2/6/6；3号胚胎3/2/2；4号胚胎2/2/3。荧光原位杂交结果显示4个胚胎均为染色体不平衡胚胎，放弃移植。结论商业化探针的合理搭配使相互易位携带者胚胎植入前诊断大为简化，因此适合绝大多数相互易位携带者。     

染色体易位携带者的胚胎植入前遗传学诊断研究进展

染色体易位是常见的染色体结构异常。应用荧光原位杂交技术，染色体易位携带者可在胚胎植入前遗传学诊断的帮助下增加正常妊娠的机会。现就相互易位减数分裂的情况进行综述，并讨论应用荧光原位杂交技术对染色体易位携带者进行胚胎植入前遗传学诊断的策略。     

柳州地区遗传咨询者罗伯逊易位核型与临床表现

目的分析罗伯逊易位与临床的关系。方法采用外周血淋巴细胞培养和染色体G显带分析,对2530例在我院接受遗传咨询者进行了染色体分析。结果共检出罗伯逊易位携带者16例,占0.63%,其中以rob（13;14）为常见（7例）,其次为rob（14;21）（5例）,成年携带者就诊原因多为流产、死胎和不育不孕,而儿童携带者多为发育异常,其中3例为罗伯逊易位21三体型。结论罗伯逊易位与流产、生育21三体型患儿密切相关,其携带者夫妇妊娠时应做产前诊断。     

FISH技术在胚胎植入前遗传学诊断中的应用及前景

随着体外受精-胚胎移植技术的快速发展和进步，以及单细胞水平上基因诊断技术的成功，使得在体外受精过程中，胚胎移植入母体子宫前进行遗传学诊断成为可能。本文综述荧光原位杂交（FISH）技术在胚胎植入前遗传学诊断（PGD）中的应用和研究进展。     

Renal dysplasia and asplenia in two sibs

A family is reported in which two sibs, one male and the other female, both died within 24 hours of birth with enlarged polycystic kidneys. Postmortem histology in the second child showed gross renal dysplasia. In both children the pancreas was enlarged, nodular and cystic but the liver appeared macroscopically normal. In the second child, histological examination confirmed pancreatic fibrosis with cystic dilation of ducts, but showed portal fibrosis with bile duct proliferation in the liver.
This combination of findings is very reminiscent of those in a girl and her brother reported by Ivemark et al. (1959). The children reported here also showed absence or hypoplasia of the spleen, cardiac anomalies and other features of the Ivemark syndrome (Ivemark 1955), a quite different, usually sporadic, congenital disorder. It is suggested that the children described here have a distinct lethal congenital disorder, probably inherited in an autosomal recessive manner.     

Schizophrenia in a North Swedish geographical isolate, 1900–1977. Epidemiology, genetics and biochemistry

Over 200 schizophrenic patients belonging to three major and interrelated pedigree complexes have been investigated over the past 30 years in a North Swedish geographically isolated population, presently numbering about 6,000. An intensive investigation of a number of biochemical correlates and genetic markers in a few selected families belonging to one of the major pedigrees has indicated new strategies for the current research program.
Schizophrenia, as defined operationally, is significantly associated with decreased activities of two enzymes (1) blood platelet monoamine oxidase, (2) plasma dopamine-β-hydroxylase, and (3) with the genetic marker Gc² (group specific antigen). Both enzymes are subject to genetic variation. A positive score for linkage between schizophrenia and low plasma DBH activity has been calculated, but, so far, available data are insufficient for discrimination between linkage and partial contribution of genetically controlled low plasma DBH to the pathogenesis of the disease. Alternatively, both mechanisms could be involved.
As a model for continued research, schizophrenia is explained as based on a double dominant-recessive genotype (Aabb), representing a vulnerability which in about 50 % of cases develops into clinical schizophrenia. It is suggested that the dominant mutation (A) operates on or affects MAO activity, and that the recessive genotype (bb) is instrumental in low variates of DBH activity and very likely such variates within the normal range of physiological variation. Moreover, it is suggested that the combined effects of MAO- and DBH-reduced efficiency on the metabolism of e.g. dopamine could be an essential pathogenic mechanism for the schizophrenic illness which is segregating in this population.     

The dominant diseases of modernized societies as omega-3 essential fatty acid deficiency syndrome: Substrate beriberi

About 1900, modern food selection and processing caused widespread $\text{epidemics}$ of the B vitamin deficiency diseases of beriberi and pellagra which, for genetic reasons, often expressed as different diseases ranging from bowel and heart disease to dermatoses and psychoses. But the B vitamins merely help convert essential fatty acids (EFA) into the prostaglandin (PG) tissue regulators and it now turns out that, through hydrogenation, milling and selection of w3-poor southern foods, we have also been systematically depleting, by as much as 90%, a newly discovered trace Nordic EFA (w3) of special importance to primates and sole precursor of the PG3(4) series, even as a concurrent fiber deficiency increases body demand for EFA. Since substrate EFA is processed by many B vitamin catalysts, an EFA deficiency will mimic a $\text{panh}$ypovitaminosis B, i.e., a mixture of $\text{substrate}$ beriberi and $\text{substrate}$ pellagra resembling vitamin beriberi and pellagra but exhibiting as even more diverse $\text{endemic}$ disease. This would consitute a second stage of the Modern Malnutrition and explain why some workers now hold the dominant diseases of modermized societies to be new, nutritionally based, pellagraform yet lipid-related and to range, once again, from heart disease to psychosis. It is an assumption that our dominant diseases are unrelated to each other or are merely revealed by our diagnostic acumen and therapeutic success; and that hydrogenating millions of tons of food oils annually, to destroy the rancidity producing w3-EFA, is safe for $\text{primates}$. Extensive beriberiform disease is reported here in 32 typical cases taken from medical practice which responds strikingly to linseed oil supplements (60% w3-EFA) in confirmation of identical results in Capuchins.     

What will studies of Fulani individuals naturally exposed to malaria teach us about protective immunity to malaria?

There are an estimated over 200 million yearly cases of malaria worldwide. Despite concerted international effort to combat the disease, it still causes approximately half a million deaths every year, the majority of which are young children with Plasmodium falciparum infection in sub-Saharan Africa. Successes are largely attributed to malaria prevention strategies, such as insecticide-treated mosquito nets and indoor spraying, as well as improved access to existing treatments. One important hurdle to new approaches for the treatment and prevention of malaria is our limited understanding of the biology of Plasmodium infection and its complex interaction with the immune system of its human host. Therefore, the elimination of malaria in Africa not only relies on existing tools to reduce malaria burden, but also requires fundamental research to develop innovative approaches. Here, we summarize our discoveries from investigations of ethnic groups of West Africa who have different susceptibility to malaria.     

'Very sore nights and days': the child's experience of illness in early modern England, c.1580-1720

Sick children were ubiquitous in early modern England, and yet they have received very little attention from historians. Taking the elusive perspective of the child, this article explores the physical, emotional, and spiritual experience of illness in England between approximately 1580 and 1720. What was it like being ill and suffering pain? How did the young respond emotionally to the anticipation of death? It is argued that children’s experiences were characterised by profound ambivalence: illness could be terrifying and distressing, but also a source of emotional and spiritual fulfilment and joy. This interpretation challenges the common assumption amongst medical historians that the experiences of early modern patients were utterly miserable. It also sheds light on children’s emotional feelings for their parents, a subject often overlooked in the historiography of childhood. The primary sources used in this article include diaries, autobiographies, letters, the biographies of pious children, printed possession cases, doctors’ casebooks, and theological treatises concerning the afterlife.     

Guidelines for the Validation and Use of Immunoassays for Determination of Introduced Proteins in Biotechnology Enhanced Crops and Derived Food Ingredients

Recent advancements in agricultural biotechnology have created a need for analytical techniques to determine introduced proteins in crops enhanced through modern biotechnology techniques. These proteins are expressed in plant tissues and may be present in food ingredients. Immunoassays are ideally suited for protein detection and may be used as both quantitative and threshold methods. Microplate ELISA and lateral flow devices are two of the most commonly used immunoassay formats for agricultural biotechnology applications. This paper provides general background information and a discussion of criteria for the validation and application of immunochemical methods to the analysis of proteins introduced into plants and food ingredients using biotechnology methods. It is the result of a collaborative effort of members of the Analytical Environmental Immunochemical Consortium. This collaborative effort represents the combined expertise of several organizations to reach consensus on establishing guidelines for the validation and use of immunoassays. Further, the paper offers developers and users a consistent approach to adopting the technology as well as aid in producing accurate and meaningful results.     

HLA in North Colombia Chimila Amerindians

HLA-A,-B,-C,-DRB1 and -DQB1 alleles have been studied in Chimila Amerindians from Sabana de San Angel (North Colombian Coast) by using high resolution molecular typing. A frequent extended haplotype was found:HLA-A*24:02-B*51:10-C*15:02-BRB1*04:07-DQB1*03:02 (28.7%) which has also been described in Amerinndian Mayos Mexican population (Mexico, California Gulf, Pacific Ocean). Other haplotypes had already been found in Amerindians from Mexico (Pacific and Atlantic Coast), Peru (highlands and Amazon Basin), Bolivia and North USA. A geographic pattern according to HLA allele or haplotype frequencies is lacking in Amerindians, as already known. Also, five new extended haplotypes were found in Chimila Amerindians. Their HLA-A*24:02 high frequencies characteristic is shared with aboriginal populations of Taiwan; also, HLA-C*01:02 high frequencies are found in New Zealand Maoris, New Caledonians and Kimberly Aborigines from Australia. Finally, this study may show a model of evolutionary factors acting and rising one HLA allele frequency (-A*24:02), but not in others that belong to the same or different HLA loci.     

Ultracryotomy: development and application (with examples from the yeast cytology) (author's transl)

The preparation steps usually necessary for obtaining ultrathin frozen sections of biological material (chemical prefixation, enclosing, cryoprotective treatment, freezing, sectioning, and post-staining the sections for transmission electron microscopy) are submitted to a critical analysis. The application of cryo-ultramicrotomy, in particularly for cytochemical purposes, is reviewed. Fundamental considerations of chemical prefixation and poststaining are supported by examples from yeast cytology. Furthermore, the efficiency of the cryo-ultramicrotomy (electron optical resolution of ultrastructural details) is demonstrated on yeast cells and protoplasts.     

The universal muscular chamber. A basic unit of the genitourinary, cardiovascular, gastro-intestinal, skeletal, cutaneous, respiratory and other systems, endocameral hypertension; and spasm, the key to their idiopathic diseases and arthropathies

Starting with the integument, we see many organs are contractile sacs or multiples thereof, which tubes or bags constitute the major part of the entire body. Recognition of this basic unit and its characteristics sheds new light, individually and collectively, on many disorders previously considered unrelated. Muscular tears and perforations develop in the walls of these chambers, being no way peculiar to those organs, wherein, hydrochloric acid occurs. So, it is not necessary to explain the absence of excessive acid from patients who exhibit holes in the gastric, uterine, aortic, duodenal, rectal, pulmonary, retina, and other walls. Muscle, not acid is the great common factor relating idiopathic disorders in the gastrointestinal tract to each other and to similar diseases in other systems. When the units are linked together, the lesions tend to appear as arthropathies, i.e. at the joints. Rephrasing common-place observations, frees us from conventional, conceptual cul-de-sacs. An observation is only as good as its interpretation, so all possibilities must be considered, otherwise, we will remain blinded by our misconceptions.