Über 27 Sippen mit infantiler amaurotischer Idiotie (Tay-Sachs)

SUMMARYThis paper is based on 45 cases in 27 families, all of which have been studied in Children Hospitals. In Switzerland almost all cases ofinfantile amaurotic idiocy (Tay-Sachs)have probably been collected, so that the stated 13 primary and 14 secondary cases may allow an estimation of the frequency of this character, which seems to oscillate temporarily. In the last 10 years no new cases have been observed.All 24 autochthonus Swiss cases are from non-Jewish, mostly rural origin, in which Eastern Jews are not to be supposed as ascendants.Our in all 27 families with TS make Slome's statistic of Jewish and non-Jewish cases in literature much more significant; the incidence of parental consanguinity is, as a matter of fact, nearly twice as high in families with non-Jewish origin.There is no evidence of a milder and longer course of TS in non-Jewish families.The mode of inheritance is, according to Slome,monohybrid autosomal recessive, though in remarkably many sibships there is an accumulation of cases. The reduction method, however, gives a percentage of 28,3 ± 6,2, coming quite near to the expectation of the Mendelian quarter.The penetrance of the character is total, the expressivity generally very equal, with only a few deviations from the well—known clinical picture of TS.The interfamiliar and intrafamiliar variability therefore is small. In not even one of the families studied have there been found other forms of lipoidosis, principally no cases ofsplenohepatomegalia Niemann-Pick. All available respective cases in Switzerland have been collected by the present author and will soon be published in these Acta. In none of these families with M.Niemann-Pickhave cases of M. Tay-Sachs been seen. This fact is liable to prove that these clinically and anatomically very similar conditions derive from independent i. e. different mutations.Modifying genes may account for the incidence of sibships in which all or almost all children died from M. TS.Environmental influences do not seem to favour its manifestations.If in the newer literature from the U.S.A. the Jewish cases of M. TS are still prevalent and if, as we heard, the concomitant manifestations occur fairly often in Israel, the origin may be sought in one at least 200 years old respective mutation in the Jewish population of a relatively restricted White-Russian era.

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CANVAS is a common form of late-onset hereditary ataxia

Nauchno-prakticheskii zhurnal «Medicinskaia genetika» ◽

10.25557/2073-7998.2020.04.51-52 ◽

2020 ◽

pp. 51-52

Author(s):

Е.П. Нужный ◽

Н.Ю. Абрамычева ◽

Е.Г. Воробьева ◽

Е.О. Иванова ◽

Ю.А. Шпилюкова ◽

...

Keyword(s):

Cerebellar Ataxia ◽

Clinical Picture ◽

Autosomal Recessive ◽

Late Onset ◽

Repeat Expansion ◽

Hereditary Ataxia ◽

Recessive Ataxia ◽

Autosomal Recessive Ataxia

Синдром CANVAS (мозжечковая атаксия, невропатия и вестибулярная арефлексия) - аутосомно-рецессивная атаксия с поздним дебютом, обусловленная носительством биаллельной экспансии (AAGGG)n во 2-м интроне гена RFC1. До настоящего момента отсутствуют сведения о распространенности данного заболевания в российских семьях. Нами был проведен поиск биаллельной экспансии AAGGG-повторов у 35 российских пациентов с поздней мозжечковой атаксией. Верифицированы 5 пациентов (14,3%) с синдромом CANVAS и характерной клинической картиной. CANVAS (cerebellar ataxia, neuropathy and vestibular areflexia) is a late-onset autosomal recessive ataxia due to biallelic (AAGGG)n repeat expansion in the 2nd intron of the RFC1 gene. There is no information on the CANVAS prevalence in Russian families. We searched for biallelic expansion of AAGGG repeats in 35 Russian patients with late-onset cerebellar ataxia. Five patients (14.3%) with CANVAS syndrome and a characteristic clinical picture were verified.

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Cystic Fibrosis Manifested as Undescended Testis and Absence of Vas Deferens

PEDIATRICS ◽

10.1542/peds.90.6.982 ◽

1992 ◽

Vol 90 (6) ◽

pp. 982-983

Author(s):

RAN GOSHEN ◽

EITAN KEREM ◽

TZIPORA SHOSHANI ◽

BAT-SHEVA KEREM ◽

ELAD FEIGIN ◽

...

Keyword(s):

Cystic Fibrosis ◽

Autosomal Recessive ◽

Undescended Testis ◽

Vas Deferens ◽

Pancreatic Insufficiency ◽

European Ancestry ◽

Inherited Disease ◽

Musculoskeletal Problems ◽

Male Patients ◽

Almost All

Cystic fibrosis (CF) is the most common autosomal recessive inherited disease in whites. Among whites of European ancestry, approximately 1 in 2000 live births are affected, implying a carrier frequency of 1:25.1 The disease is characterized by chronic lung disease, which usually leads to the patient's death. Furthermore, patients with CF suffer from pancreatic insufficiency and other less common manifestations, such as meconium ileus, hepatobiliary abnormalities, diabetes mellitus, and musculoskeletal problems.1 Almost all males with CF are infertile. Absence of the vas deferens has been reported in 70% to more than 90% of male patients affected by CF.2 Although 4% of full-term male neonates have un-descended testes at birth, 0.8% to 1.0% of 1-year-old boys have cryptorchism and may be subjected to a later surgical intervention.3

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Characterising the phenotype and mode of inheritance of patients with inherited peripheral neuropathies carrying MME mutations

Journal of Medical Genetics ◽

10.1136/jmedgenet-2018-105650 ◽

2018 ◽

Vol 55 (12) ◽

pp. 814-823 ◽

Cited By ~ 8

Author(s):

Vincenzo Lupo ◽

Marina Frasquet ◽

Ana Sánchez-Monteagudo ◽

Ana Lara Pelayo-Negro ◽

Tania García-Sobrino ◽

...

Keyword(s):

Autosomal Recessive ◽

Late Onset ◽

Axonal Neuropathy ◽

Genetic Diagnosis ◽

Hereditary Neuropathy ◽

Motor Neuropathy ◽

Charcot Marie Tooth Disease ◽

Hereditary Motor Neuropathy ◽

Index Cases ◽

Mode Of Inheritance

BackgroundMutations in the metalloendopeptidase (MME) gene were initially identified as a cause of autosomal recessive Charcot-Marie-Tooth disease type 2 (CMT2). Subsequently, variants in MME were linked to other late-onset autosomal dominant polyneuropathies. Thus, our goal was to define the phenotype and mode of inheritance of patients carrying changes in MME.MethodsWe screened 197 index cases with a hereditary neuropathy of the CMT type or distal hereditary motor neuropathy (dHMN) and 10 probands with familial amyotrophic lateral sclerosis (fALS) using a custom panel of 119 genes. In addition to the index case subjects, we also studied other clinically and/or genetically affected and unaffected family members.ResultsWe found 17 variants in MME in a total of 20 index cases, with biallelic MME mutations detected in 13 cases from nine families (three in homozygosis and six in compound heterozygosis) and heterozygous variants found in 11 families. All patients with biallelic variants had a similar phenotype, consistent with late-onset axonal neuropathy. Conversely, the phenotype of patients carrying heterozygous mutations was highly variable [CMT type 1 (CMT1), CMT2, dHMN and fALS] and mutations did not segregate with the disease.ConclusionMME mutations that segregate in an autosomal recessive pattern are associated with a late-onset CMT2 phenotype, yet we could not demonstrate that MME variants in heterozygosis cause neuropathy. Our data highlight the importance of establishing an accurate genetic diagnosis in patients carrying MME mutations, especially with a view to genetic counselling.

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Genetic hearing loss: a study of 228 Brazilian patients

Genetics and Molecular Biology ◽

10.1590/s1415-47572000000100004 ◽

2000 ◽

Vol 23 (1) ◽

pp. 25-27 ◽

Cited By ~ 3

Author(s):

Silvia Bragagnolo Longhitano ◽

Décio Brunoni

Keyword(s):

Hearing Loss ◽

Autosomal Recessive ◽

Autosomal Dominant ◽

Autosomal Recessive Inheritance ◽

Recessive Inheritance ◽

Dominant Inheritance ◽

Genetic Etiology ◽

Parental Consanguinity ◽

Genetic Hearing Loss ◽

Associated Abnormalities

We studied 228 patients, with suspected or confirmed genetic hearing loss, in order to determine the clinical and genetic diagnoses and etiology of each case. Deafness with no associated abnormalities was found in 146 patients (64%) belonging to 112 families. Syndromic deafness was diagnosed in 82 patients (36%) belonging to 76 families. The genetic etiology was as follows: autosomal recessive inheritance in 40.8% of syndromics and non-syndromics, autosomal dominant inheritance in 13.2% and X-linked recessive in 1.3%. In 44.7% of the cases, the etiology of the hearing loss could not be determined. Monogenic causes are the most possible etiology in the latter cases. Parental consanguinity was found in 22.4% of the cases, and deafness was bilateral, profound and neurosensorial in 47.4% of the patients. An early onset of hearing loss (< 2 years of age) occurred in 46.5% of the cases. These results are similar to previous literature reports.

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Pyloroduodenal Atresia (Diaphragm Type): An Autosomal Recessive Disease

PEDIATRICS ◽

10.1542/peds.62.3.419 ◽

1978 ◽

Vol 62 (3) ◽

pp. 419-421

Author(s):

Henry C. Mishalany ◽

Ziad H. Idriss ◽

Vazken M. Der Kaloustian

Keyword(s):

Autosomal Recessive ◽

Autosomal Recessive Disease ◽

Single Individual ◽

Autosomal Recessive Mode ◽

Genetic Etiology ◽

New Evidence ◽

Mode Of Inheritance

In 1970,1 1971,2 and 19743 we described two families, each with two siblings who had atresia of the first portion of the duodenum. The four patients were first cousins to each other. We suggested a genetic etiology with an autosomal recessive mode of inheritance, which has been accepted.4 The source of the proposed gene for both families was traced to a single individual. Recently, a third family, linked to the previous two with strong consanguineous ties, had a pair of twins affected with the same anomaly. The purpose of this article is to bring the weight of new evidence afforded by this third family to further substantiate the genetic etiology of this condition.

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THE ICHTHYOSIFORM DERMATOSES

PEDIATRICS ◽

10.1542/peds.42.6.990 ◽

1968 ◽

Vol 42 (6) ◽

pp. 990-1004

Author(s):

Nancy B. Esterly

Keyword(s):

Autosomal Recessive ◽

Autosomal Dominant ◽

Clinical Investigation ◽

Correct Diagnosis ◽

Associated Anomalies ◽

Dominant Trait ◽

Autosomal Dominant Trait ◽

Clinical Variants ◽

Congenital Ichthyosiform Erythroderma ◽

Mode Of Inheritance

The Term ichthyosis describes a group of heritable disorders which are characterized by cutaneous scaling. The visible scale differentiates these disorders from xeroderma in which the skin is dry but does not visibly desquamate. Many classifications of the ichthyoses have been proposed, but most are descriptive and contribute little to an understanding of etiology and pathogenesis. Often clinical variants or patients with minor associated anomalies have been categorized separately on an empirical basis and, in some cases, several names have been used for one entity to indicate severity of involvement. The most useful classification appears to be that of Wells and Kerr,1 who segregated the various types by their pattern of inheritance and retained the nomenclature in common usage. Differences in clinical features and histologic patterns also correlate with these genetically distinguishable types. Thus, with careful attention to the distribution and type of scale, family history, and skin histology, the physician will be able to classify patients in a meaningful way. Such an approach is helpful for several reasons. The prognosis, troublesome features, and degree of handicapping differ for the various ichthyoses. Sensible genetic counseling, an important part of the management of such patients, is possible only with the correct diagnosis. Moreover, clinical investigation of affected individuals will be further confused unless the entity under study is well defined. The need for an understanding of the physiologic and biochemical defects of ichthvotic skin is underscored by the limitations of currently available therapy. The four major types of ichthyosis include: (1) ichthyosis vulgaris, transmitted as an autosomal dominant trait; (2) sexlinked ichthyosis, transmitted as an Xlinked trait; (3) bullous congenital ichthyosiform erythroderma (CIE), inherited as an autosomal dominant trait; and (4) nonbulbus congenital ichthyosiform erythroderma, autosomal recessive mode of inheritance (Table I).

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Bi-allelic SHOC1 loss-of-function mutations cause meiotic arrest and non-obstructive azoospermia

Journal of Medical Genetics ◽

10.1136/jmedgenet-2020-107042 ◽

2020 ◽

pp. jmedgenet-2020-107042

Author(s):

Chencheng Yao ◽

Chao Yang ◽

Liangyu Zhao ◽

Peng Li ◽

Ruhui Tian ◽

...

Keyword(s):

Autosomal Recessive ◽

Periodic Acid ◽

Compound Heterozygous ◽

Obstructive Azoospermia ◽

Autosomal Recessive Mode ◽

Loss Of Function ◽

Meiotic Arrest ◽

Causative Gene ◽

Periodic Acid Schiff ◽

Mode Of Inheritance

BackgroundThe genetic causes of human idiopathic non-obstructive azoospermia (NOA) with meiotic arrest remain unclear.MethodsTwo Chinese families with infertility participated in the study. In family 1, two brothers were affected by idiopathic NOA. In family 2, the proband was diagnosed with idiopathic NOA, and his elder sister suffered from infertility. Whole-exome sequencing (WES) was conducted in the two patients in family 1, the proband in family 2 and 362 additional sporadic patients with idiopathic NOA. Sanger sequencing was used to verify the WES results. Periodic acid–Schiff (PAS), immunohistochemistry (IHC) and meiotic chromosomal spread analyses were carried out to evaluate the stage of spermatogenesis arrested in the affected cases.ResultsWe identified compound heterozygous loss of function (LoF) variants of SHOC1 (c.C1582T:p.R528X and c.231_232del:p.L78Sfs*9, respectively) in both affected cases with NOA from family 1. In family 2, homozygous LoF variant in SHOC1 (c.1194delA:p.L400Cfs*7) was identified in the siblings with infertility. PAS, IHC and meiotic chromosomal spread analyses demonstrated that the spermatogenesis was arrested at zygotene stage in the three patients with NOA. Consistent with the autosomal recessive mode of inheritance, all of these SHOC1 variants were inherited from heterozygous parental carriers. Intriguingly, WES of 362 sporadic NOA cases revealed one additional NOA case with a bi-allelic SHOC1 LoF variant (c.1464delT:p.D489Tfs*13).ConclusionTo the best of our knowledge, this is the first report identifying SHOC1 as the causative gene for human NOA. Furthermore, our study showed an autosomal recessive mode of inheritance in the NOA caused by SHOC1 deficiency.

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Glycoprotein-180 deficiency: genetics and abnormal neutrophil activation

Blood ◽

10.1182/blood.v65.3.696.696 ◽

1985 ◽

Vol 65 (3) ◽

pp. 696-704 ◽

Cited By ~ 14

Author(s):

SJ Weisman ◽

RL Berkow ◽

G Plautz ◽

M Torres ◽

WA McGuire ◽

...

Keyword(s):

Autosomal Recessive ◽

Transmembrane Potential ◽

Neutrophil Function ◽

Surface Glycoprotein ◽

Receptor Density ◽

Myristate Acetate ◽

Wool Fibers ◽

C3b Receptor ◽

Mode Of Inheritance ◽

Made In

Abstract Neutrophil function was studied in a patient with polymorphonuclear leukocyte (PMN) glycoprotein-180 deficiency and in her parents. PMNs of the patient had abnormal chemotaxis, phagocytosis, adherence, surface charge, and membrane-associated events of activation. Selective defects to C3b, immunoglobulin G (IgG), phorbol myristate acetate (PMA) and N- formyl-methionyl-leucyl-phenylalanine (FMLP) are described, although C3b receptor density was normal. The parents were found to have abnormal adherence to nylon-wool fibers, abnormal transmembrane potential depolarization with PMA, and reduced amounts of glycoprotein- 180 in their PMNs. These studies provide further evidence that the oxidative burst has several different pathways for activation. They demonstrate that the absence of a single PMN surface glycoprotein is associated with a broad spectrum of PMN functional abnormalities. Finally, the observations made in the parents support an autosomal recessive mode of inheritance.

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Genetic inheritance pattern in prurigo Hebra

Paediatrica Indonesiana ◽

10.14238/pi41.2.2001.76-81 ◽

2001 ◽

Vol 41 (2) ◽

pp. 76

Author(s):

Siti Aisah Boediardja ◽

Wahyuning Ramelan ◽

Santoso Cornain

Keyword(s):

Autosomal Recessive ◽

Morbidity Rate ◽

Inheritance Pattern ◽

Genetic Inheritance ◽

Chi Square ◽

Chi Square Test ◽

Lower Morbidity ◽

Mode Of Inheritance ◽

Rule Out

A study was conducted to analyze the multifactorial genetic inheritance pattern in prurigo Hebra (PH). Fiftyprobands (PH patients) consisting of 11 males and 39 females, with age ranged from 5-30 years were included in this study.A three-generation family tree was obtained from each subject, from which a total of 79 families were eligible for analysis. Foreach family the possible mode of inheritance, namely autosomal dominant (AD) or autosomal recessive (AR), was predicted.The families were then grouped according to the mode of inheritance. Analysis was conducted using Chi-square test,comparing the observed occurrence of PH and the expected value for each mode. To rule out mutation, the second methodwas applied, which only families with more than one affected child were analyzed, was used. The genetic inheritancepattern was not consistently compatible either with AR or AD. This finding, and other supporting facts, such as femalepreponderace, the role of HLA and the lower morbidity rate compared to the expected rate in AR or AD mode, indicated thatthe genetic inheritance of PH follows a multi-factorial pattern.

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The Detection of Carriers in Hereditary Myoclonic Epilepsy

Acta geneticae medicae et gemellologiae ◽

10.1017/s1120962300018199 ◽

1960 ◽

Vol 9 (4) ◽

pp. 466-471 ◽

Cited By ~ 4

Author(s):

M. Bruce Sarlin ◽

H. Warner Kloepfer ◽

Walter A. Mickle ◽

Robert G. Heath

Keyword(s):

Autosomal Recessive ◽

Similar Type ◽

Myoclonic Epilepsy ◽

Autosomal Recessive Mode ◽

Negro Family ◽

Heterozygous Carriers ◽

Mode Of Inheritance

SummaryThree cases of hereditary myoclonic epilepsy have been observed among ten siblings in a Negro family. Electroencephalograms of the parents, three normal siblings and two of the three affected siblings have been recorded and all show abnormalities of a similar type. These are of a generalized nature revealing no focal damage. This type of abnormality has been observed in an affected male and two normal siblings by Watson and Denny-Brown.The autosomal recessive mode of inheritance observed in the present study is consistent with the transmission most frequently reported in myoclonic epilepsy. We believe that abnormal electroencephalographic patterns are associated with this gene and that these patterns may be useful in the detection of heterozygous carriers.

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