Your search keyword '"family study"' showing total 1,045 results

1. Verbal fluency in schizophrenia and bipolar disorder - A longitudinal, family study

Author

Luperdi, Sussy C., Correa-Ghisays, Patricia, Vila-Francés, Joan, Selva-Vera, Gabriel, Livianos, Lorenzo, Tabarés-Seisdedos, Rafael, and Balanzá-Martínez, Vicent

Published

2024

2. Three Fields Allelic Haplotype Frequencies of HLA‐DPA1 and ‐DPB1 Typed by Next Generation Sequencing of 563 Families in Chinese Han Population.

Author

Wang, Jian‐Ling, He, Jun‐Bo, Li, Zhi‐Min, Zhu, Ya‐Nan, Cao, DaJiang, Fu, Hong‐Lei, Zhang, Xian, Fernández‐Viña, Marcelo A., Rozemuller, Erik, and Liu, XiangJun

Subjects

*HEMATOPOIETIC stem cell transplantation, *NUCLEOTIDE sequencing, *CHINESE people, *HAPLOTYPES, *NUCLEAR families

Abstract

The present study investigated the HLA‐DPA1 and ‐DPB1 allele and haplotype frequencies in the Chinese Han population. A total of 563 families, which have been typed for the purpose of haematopoietic stem cell transplantation, were included, and three‐field allelic resolution typing of HLA‐DPA1 and ‐DPB1 of all individuals were defined by the next‐generation sequencing method. HLA‐DPA1~DPB1 haplotypes were determined by allele segregation within a nuclear family. A total of 9 HLA‐DPA1 and 39 HLA‐DPB1 alleles, and 62 HLA‐DPA1~DPB1 haplotypes were identified. The three most frequent alleles at HLA‐DPA1 locus are HLA‐DPA1*02:02:02 (46.581%), HLA‐DPA1*01:03:01 (36.456%) and HLA‐DPA1*02:01:01 (12.167%); and the three most frequent HLA‐DPB1 alleles are HLA‐DPB1*05:01:01 (34.014%), HLA‐DPB1*02:01:02 (18.428%) and HLA‐DPB1*04:01:01 (10.124%). The three most frequent haplotypes are HLA‐DPA1*02:02:02~DPB1*05:01:01 (32.327%), HLA‐DPA1*01:03:01 ~ DPB1*02:01:02 (14.654%) and HLA‐DPA1*01:03:01~DPB1*04:01:01 (9.458%). The HLA‐DPA1*02:01~DPB1*02:02 and HLA‐DPA1*04:01~DPB1*05:01 haplotypes appear to be unique in Han Chinese. Strong global linkage disequilibrium (LD) between HLA‐DPA1 and ‐DPB1 was confirmed (D′ = 0.848, Wn = 0.684). Moreover, the haplotype frequencies based on the family study were compared with the frequencies estimated by the expectation–maximisation algorithm, and the equivalent results were obtained except for haplotypes with very low frequencies. Our data provide a solid base for HLA‐DP dimer association studies and useful information for transplantation and disease association studies. [ABSTRACT FROM AUTHOR]

Published

2024

3. Like Mother, Like Daughter? Double Standards in Body Evaluation and Their Familial Transmission in Female Adolescents and Their Mothers.

Author

Quittkat, Hannah L., Voges, Mona M., Düsing, Rainer, Schöne, Benjamin, and Vocks, Silja

Subjects

*TEENAGE girls, *FAT, *BODY image, *DOUBLE standard, *EATING disorders

Abstract

Background: Cognitive biases, such as applying stricter body evaluation for oneself than for others, are presumed to promote the development and maintenance of eating disorders. While questionnaire data have demonstrated a familial transmission of body image, these self-deprecating double standards (DS) have not been studied among female adolescents, and a potential familial transmission of DS through feedback/role-modeling is yet to be explored. The present study thus addresses these questions. Methods: Female adolescents and their mothers viewed pictures of their own and peer bodies presented with their own and another peer's face, and were asked to rate arousal, valence, body attractiveness, and body fat for each body. Results: Daughters evaluated their own, an average-weight, and an overweight build as less attractive and with more body fat when presented with their own than with another face, while mothers mainly applied such self-deprecating DS for an overweight build. Regarding familial transmission, higher negative maternal feedback was associated with more self-deprecating DS of body fat and attractiveness in daughters when viewing an overweight build. Conclusions: Female adolescents and their mothers apply self-deprecating DS, suggesting that DS are widespread. Psychoeducation and training regarding communication, feedback, and body functionality might support the prevention of DS. [ABSTRACT FROM AUTHOR]

Published

2024

4. Prevalence and Determinants of Liver Disease in Relatives of Italian Patients With Advanced MASLD.

Author

Pelusi, Serena, Ronzoni, Luisa, Rondena, Jessica, Rosso, Chiara, Pennisi, Grazia, Dongiovanni, Paola, Margarita, Sara, Carpani, Rossana, Soardo, Giorgio, Prati, Daniele, Cespiati, Annalisa, Petta, Salvatore, Bugianesi, Elisabetta, and Valenti, Luca

Abstract

Metabolic dysfunction associated steatotic liver disease (MASLD) has a strong genetic component. The aim of this study was to examine noninvasively the prevalence of MASLD and of advanced fibrosis in relatives of patients with advanced MASLD and the risk factors for liver involvement, with a focus on the contribution of common genetic risk variants. We prospectively enrolled 98 consecutive probands with advanced fibrosis and/or hepatocellular carcinoma caused by MASLD and 160 nontwin first-degree relatives noninvasively screened for MASLD and advanced fibrosis at 4 Italian centers. We evaluated common genetic determinants and polygenic risk scores of liver disease. Among relatives, prevalence of MASLD was 56.8% overall, whereas advanced fibrosis was observed in 14.4%. At multivariable analysis in relatives, MASLD was associated with body mass index (odds ratio [OR], 1.31 [1.18–1.46]) and tended to be associated with diabetes (OR, 5.21 [0.97–28.10]), alcohol intake (OR, 1.32 [0.98–1.78]), and with female sex (OR, 0.54 [0.23–1.15]), whereas advanced fibrosis was associated with diabetes (OR, 3.13 [1.16–8.45]) and nearly with body mass index (OR, 1.09 [1.00–1.19]). Despite that the PNPLA3 risk variant was enriched in probands (P =.003) and overtransmitted to relatives with MASLD (P =.045), evaluation of genetic risk variants and polygenic risk scores was not useful to guide noninvasive screening of advanced fibrosis in relatives. We confirmed that about 1 in 7 relatives of patients with advanced MASLD has advanced fibrosis, supporting clinical recommendations to perform family screening in this setting. Genetic risk variants contributed to liver disease within families but did not meaningfully improve fibrosis risk stratification. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

5. Identification of a pathogenic SDHD mutation in a Chinese family with hereditary head and neck paraganglioma: implications for genetic counseling and management

Author

Pu Wang, Liming Gao, Wenyang Zhang, Rui Guo, and Yin Xia

Subjects

SDHD mutation, Hereditary head and neck paraganglioma, Genetic counseling, Family study, Whole exome sequencing, Surgery, RD1-811, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background This study aims to identify a pathogenic SDHD mutation associated with hereditary head and neck paraganglioma (HNPGL) in a Chinese family and to explore its implications for genetic counseling. Methods The study involved a family with 15 members spanning three generations. A 31-year-old patient (II-4) was diagnosed with a left parotid gland tumor and a right carotid body tumor, while both the father and elder sister had right carotid body tumors, and the third sister had bilateral carotid body tumors. Whole exome sequencing and Sanger sequencing were employed to identify candidate pathogenic variants. Genetic counseling was conducted for third-generation descendants to assess the likelihood of carrying the mutation and to guide future diagnosis and treatment. Results A nonsense mutation in the SDHD gene (NM_001276503:exon2:c.C64T: p.R22X) was identified in the patient and three other affected family members. Genetic counseling for the third generation revealed that only one child (III-4) carried the pathogenic mutation inherited from the patient’s third sister. Conclusion We identified a pathogenic mutation in SDHD in a Chinese HNPGL family, which is the second reported case of its kind. Our genetic counseling analysis for the third generation provided important information for the family and guidance for future diagnosis and treatment.

Published

2025

6. A Family Study of Executive Function in Gambling Disorder.

Author

Aidelbaum, Robert, Hodgins, David C., and Goghari, Vina M.

Subjects

*EXECUTIVE function, *COMPULSIVE gambling, *REWARD (Psychology), *RESPONSE inhibition, *DELAY of gratification

Abstract

Impulsivity-characterized executive function impairments have been hypothesized to represent mechanisms underlying the symptomology associated with gambling disorder (GD). Despite this, a clear profile of executive function within GD has yet to be established. Furthermore, it remains unclear whether executive function deficits represent a vulnerability marker for the disorder. This study assessed executive function performance within a GD sample compared to a sample of familial relatives and community controls. Using a family study methodology, a broad assessment of executive function was administered to analyze performance differences and their potential characterization by impulsivity between a sample of individuals meeting criteria for GD, their first-degree familial relatives, and a community control sample. Performance differences emerged regarding the capacity to delay gratification and inhibit automatic task-irrelevant responses between the GD and control samples. Results support the presence of impulsive choice and impulsive cognitive bias as components of the GD executive functioning profile. Similar difficulties inhibiting automatic attentional shifting were observed within the first-degree relative sample. Executive functioning within GD appears to be characterized by an impulsive pattern of behaviours/decisions but impacts processes differently. Evidence suggests that individuals diagnosed with GD demonstrate a statistically different capacity to delay gratification (e.g. a propensity towards smaller, more immediate rewards as opposed to larger delayed rewards) and inhibit cognitive biases (e.g. difficulty shifting attention away from task-irrelevant stimuli). This latter difference may represent a vulnerability marker of GD as preliminary evidence was provided for similar difficulties in a first-degree relative sample. Further research must replicate these findings and assess the impact of task modality, symptom severity, and comorbidity on the observation of executive functioning impairment. [ABSTRACT FROM AUTHOR]

Published

2024

7. Cognitive impairment in 'non‐user' first‐degree relatives of persons with cannabis dependence syndrome: A pilot, endophenotype study.

Author

Das, Shrayasi, Singh, Lokesh Kumar, Tikka, Sai Krishna, Spoorthy, Mamidipalli Sai, Mandal, Sucharita, Soni, Puneet Kumar, and Nandan, Neethu K.

Subjects

*EXECUTIVE function, *MARIJUANA abuse, *COGNITION disorders, *RELATIVES, *COGNITIVE ability, *PATIENT-family relations, *DRUG withdrawal symptoms

Abstract

Introduction: Cannabis use disorders are global emerging problem nowadays, with high prevalence and morbidity. Cognitive impairments, and also corresponding genetic vulnerability, has been fairly replicated in individuals with cannabis dependence. However, there are few studies that assess cognitive functioning as an endophenotype or a trait marker for cannabis dependence. While the primary objective of this study was to assess the endophenotype pattern of cognitive dysfunction in cannabis dependence, assessing the association between the degree of cognitive functioning, and their socio‐demographic and clinical variables in the cannabis dependence patients and their first‐degree relatives was the secondary objective. Methodology: We compared cognitive functioning across three groups‐ patients with cannabis dependence syndrome, their 'non‐user' first‐degree relatives and healthy controls, with 30 participants in each group. Five cognitive domains‐ attention and concentration, verbal fluency, memory, visuospatial ability and executive functions were assessed. We assessed for endophenotype pattern of statistical significance in pairwise analyses of Kruskal‐Wallis test, which was corrected for multiple comparisons. Subsequently, correlation analysis to assess association of cognitive impairment with socio‐demographic and clinical variables was conducted. Results: Although impairment in attention and executive functions also was seen in patients with cannabis dependence, endophenotype pattern of statistical significance in pairwise analyses, with impairment in first‐degree relatives too, was seen in all sub‐scores of verbal fluency and verbal memory. None of the correlations were significant. Conclusion: 'Non‐user' first‐degree relatives of patients with cannabis dependence too show significant cognitive impairment. Verbal fluency and verbal memory are possible endophenotypes or trait markers for cannabis dependence syndrome. [ABSTRACT FROM AUTHOR]

Published

2024

8. Usroh

Subjects

islamic family law, family study, legal drafting of islamic civil law, customary law, inheritance law, marriage and gender, Islamic law, KBP1-4860

Published

2024

9. A Family-Based Study of Inherited Genetic Risk in Lipedema.

Author

Morgan, Steven, Reid, Isabella, Bendon, Charlotte, Ishaq, Musarat, Shayan, Ramin, Pope, Bernard, Park, Daniel, and Karnezis, Tara

Abstract

Background: Lipedema is a progressive condition involving excessive deposition of subcutaneous adipose tissue, predominantly in the lower limbs, which severely compromises quality of life. Despite the impact of lipedema, its molecular and genetic bases are poorly understood, making diagnosis and treatment difficult. Historical evaluation of individuals with lipedema indicates a positive family history in 60%–80% of cases; however, genetic investigation of larger family cohorts is required. Here, we report the largest family-based sequencing study to date, aimed at identifying genetic changes that contribute to lipedema. Methods and Results: DNA samples from 31 individuals from 9 lipedema families were analyzed to reveal genetic variants predicted to alter protein function, yielding candidate variants in 469 genes. We did not identify any individual genes that contained likely disease-causing variants across all participating families. However, gene ontology analysis highlighted vasopressin receptor activity, microfibril binding, and patched binding as statistically significantly overrepresented categories for the set of candidate variants. Conclusions: Our study suggests that lipedema is not caused by a single exomic genetic factor, providing support for the hypothesis of genetic heterogeneity in the etiology of lipedema. As the largest study of its kind in the lipedema field, the results advance our understanding of the disease and provide a roadmap for future research aimed at improving the lives of those affected by lipedema. [ABSTRACT FROM AUTHOR]

Published

2024

10. Characterization of D4Z4 alleles and assessment of de novo cases in Facioscapulohumeral dystrophy (FSHD) in a cohort of Italian families.

Author

Strafella, Claudia, Colantoni, Luca, Megalizzi, Domenica, Trastulli, Giulia, Piorgo, Emma Proietti, Primiano, Guido, Sancricca, Cristina, Ricci, Giulia, Siciliano, Gabriele, Caltagirone, Carlo, Filosto, Massimiliano, Tasca, Giorgio, Ricci, Enzo, Cascella, Raffaella, and Giardina, Emiliano

Abstract

Facioscapulohumeral dystrophy (FSHD) is an autosomal dominant disease, although 10%–30% of cases are sporadic. However, this percentage may include truly de novo patients (carrying a reduced D4Z4 allele that is not present in either of the parents) and patients with apparently sporadic disease resulting from mosaicism, non‐penetrance, or complex genetic situations in either patients or parents. In this study, we characterized the D4Z4 Reduced Alleles (DRA) and evaluated the frequency of truly de novo cases in FSHD1 in a cohort of DNA samples received consecutively for FSHD‐diagnostic from 100 Italian families. The D4Z4 testing revealed that 60 families reported a DRA compatible with FSHD1 (1–10 RU). The DRA co‐segregated with the disease in most cases. Five families with truly de novo cases were identified, suggesting that this condition may be slightly lower (8%) than previously reported. In addition, D4Z4 characterization in the investigated families showed 4% of mosaic cases and 2% with translocations. This study further highlighted the importance of performing family studies for clarifying apparently sporadic FSHD cases, with significant implications for genetic counseling, diagnosis, clinical management, and procreative choices for patients and families. [ABSTRACT FROM AUTHOR]

Published

2024

11. The multi-generational familial aggregation of interstitial cystitis, other chronic nociplastic pain disorders, depression, and panic disorder.

Author

Allen-Brady, Kristina, Fyer, Abby J., and Weissman, Myrna

Subjects

*MENTAL depression risk factors, *CHRONIC pain, *IRRITABLE colon, *PANIC disorders, *FIBROMYALGIA, *RISK assessment, *DISEASE susceptibility, *RESEARCH funding, *DESCRIPTIVE statistics, *MEDICAL records, *INTERSTITIAL cystitis, *CHRONIC fatigue syndrome, *DISEASE risk factors

Abstract

Background: Interstitial cystitis/painful bladder syndrome (IC) is a chronic pelvic pain condition which has high comorbidity with other nociplastic, or unexplained, pain disorders [e.g. fibromyalgia (FM), irritable bowel syndrome (IBS), and myalgic encephalomyelitis/chronic fatigue (ME/CFS)] and some psychiatric conditions [major depressive disorder (MDD) and panic disorder (PD)]. Here we investigated the shared familiality of IC and these other nociplastic and psychiatric conditions. Methods: Subjects were identified in the Utah Population Database, which links genealogy data back to the 1800s to medical record diagnosis billing code data back to 1995. We computed the relative risk of each of these disorders among first (FDR), second (SDR), and third-degree relatives (TDR) of six proband groups: IC, FM, IBS, ME/CFS, PD, and MDD. Given the known familial aggregation of each of these disorders, we conducted our analyses to test for heritable interrelationships using proband subgroups whose members did not have the diagnosis assessed in their relatives. Results: We observed strong evidence for heritable interrelationships among all six disorders. Most analyses indicated significantly increased risk for each of the six disorders in FDR, SDR, and TDR of all or most proband groups. Out of 30 possible bidirectional disorder interrelationships, 26 were significant among FDR, 23 were significant among SDR, and 7 were significant among TDR. Clustering was observed in both close and distant relatives. Conclusions: Our results support a common, heritable component to IC and other nociplastic and psychiatric conditions. [ABSTRACT FROM AUTHOR]

Published

2023

12. Analysis of secondary failure time responses in studies with response‐dependent sampling schemes.

Author

Zhong, Yujie, Cook, Richard J., and Yu, Aiai

Subjects

*FAILURE analysis, *SECONDARY analysis, *PSORIATIC arthritis, *KINSHIP, *STATISTICS

Abstract

Response‐dependent sampling is routinely used as an enrichment strategy in the design of family studies investigating the heritable nature of disease. In addition to the response of primary interest, investigators often wish to investigate the association between biomarkers and secondary responses related to possible comorbidities. Statistical analysis regarding genetic biomarkers and their association with the secondary outcome must address the biased sampling scheme involving the primary response. In this article, we develop composite likelihoods and two‐stage estimation procedures for such secondary analyses in which the within‐family dependence structure for the primary and secondary outcomes is modeled via a Gaussian copula. The dependence among responses within family members is modeled based on kinship coefficients. Auxiliary data from independent individuals are exploited by augmenting the composite likelihoods to increase precision of marginal parameter estimates and enhance the efficiency of estimators of the dependence parameters. Simulation studies are carried out to evaluate the finite sample performance of the proposed method, and an application to a motivating family study in psoriatic arthritis is given for illustration. [ABSTRACT FROM AUTHOR]

Published

2023

13. Postmortem genetic analysis of 17 sudden cardiac deaths identified nonsense and frameshift variants in two cases of arrhythmogenic cardiomyopathy.

Author

Takahashi, Yoichiro, Fukuda, Haruki, Hayakawa, Akira, Sano, Rie, Kubo, Rieko, Kawabata-Iwakawa, Reika, Nakajima, Tadashi, Ishige, Takashi, Tokue, Hiroyuki, Asano, Kazuya, Seki, Tomohiro, Hsiao, Yi-Yang, Ishizawa, Fujio, Takei, Hiroyuki, and Kominato, Yoshihiko

Subjects

*CARDIAC arrest, *AUTOPSY, *POSTMORTEM changes, *BRUGADA syndrome, *CORONARY disease, *SUDDEN death, *CARDIOMYOPATHIES, *SUDDEN onset of disease

Abstract

Sudden death, or unexpected natural death of a healthy individual, is a serious problem in all nations. Sudden cardiac death (SCD) mainly due to ischemic heart diseases is the top cause of sudden death. However, there are pathophysiological conditions, referred to as sudden arrhythmic death syndrome, in which no apparent lesion can be identified even after complete conventional or ordinary autopsy. While postmortem genetic analyses have accumulated evidence about underlying genetic abnormality in such cases, the precise relationships between genetic background and the phenotype have been largely elusive. In this study, a retrospective investigation of 17 autopsy cases in which lethal arrhythmia was suspected to be the cause of death was carried out. Genetic analysis focusing on 72 genes reported to be associated with cardiac dysfunctions was performed, in combination with detailed histopathological and postmortem imaging examination, and a family study. As a result, in two cases of suspected arrhythmogenic cardiomyopathy (ACM), we found a nonsense variant in PKP2 and frameshift variant in TRPM4 gene. In contrast, the other 15 cases showed no morphological changes in the heart despite the presence of a frameshift variant and several missense variants, leaving the clinical significance of these variants obscure. The findings of the present study suggest that nonsense and frameshift variants could be involved in the morphological abnormality in cases of SCD due to ACM, while missense variants alone rarely contribute to massive structural changes in the heart. [ABSTRACT FROM AUTHOR]

Published

2023

14. Exploring risk factors and transmission dynamics of Hepatitis B infection among Indian families: Implications and perspective

Author

Shreyasi Athalye, Naveen Khargekar, Shailesh Shinde, Tejashwini Parmar, Shreya Chavan, Ganeshmoorthy Swamidurai, Vaishali Pujari, Priyanka Panale, Priyanka Koli, Aruna Shankarkumar, and Anindita Banerjee

Subjects

Hepatitis B virus (HBV), Intrafamilial transmission, Risk factors, Occult Hepatitis B, OBI, Family study, Infectious and parasitic diseases, RC109-216, Public aspects of medicine, RA1-1270

Abstract

Introduction: Hepatitis B virus (HBV) is global health problem. Family members of HBV infected people are considered as high-risk groups due to frequent household transmission of HBV among contacts of HBsAg carriers. The present study aimed to investigate the intrafamilial transmission of HBV among family members of HBV-infected persons and to identify the risk factors for viral transmission in these setting. Methods: 361 index cases and their 1083 family contacts were tested for markers of Hepatitis B, viz. HBsAg and HBcAb using commercial ELISA. The demographic details and risk factors for acquiring HBV infection among the family members were recorded using a structured questionnaire. Results: The median (IQR) age of index cases and family members was 37 (27 − 48) and 26 (14 − 38) years, respectively. Among the screened family members, 9.23% (n = 100) members were positive for HBsAg and 32.75% (n = 355) were positive for HBcAb. At least one member of the family was affected in 229/361 (63.43%) index cases. Significantly lower percent of household contacts (9.23%, n = 100)were vaccinated against HBV.HBV transmission risk was significantly higher in families with more than four members(p

Published

2023

15. Genome-wide DNA methylation analysis in families with multiple individuals diagnosed with schizophrenia and intellectual disability.

Author

Zhang, Shengmin, Shi, Kaiyu, Lyu, Nan, Zhang, Yunshu, Liang, Guangming, Zhang, Wufang, Wang, Xijin, Wen, Hong, Wen, Liping, Ma, Hong, Wang, Jijun, Yu, Xin, and Guan, Lili

Subjects

*DNA methylation, *INTELLECTUAL disabilities, *DNA analysis, *PEOPLE with schizophrenia, *TWINS

Abstract

Schizophrenia (SZ) and intellectual disability (ID) are both included in the continuum of neurodevelopmental disorders (NDDs). DNA methylation is known to be important in the occurrence of NDDs. The family study is conducive to eliminate the effects of relative epigenetic backgrounds, and to screen for differentially methylated positions (DMPs) and regions (DMRs) that are truly associated with NDDs. Four monozygotic twin families were recruited, and both twin individuals suffered from NDDs (either SZ, ID, or SZ plus ID). Genome-wide methylation analysis was performed in all samples and each family. DMPs and DMRs between NDD patients and unaffected individuals were identified. Functional and pathway enrichment analyses were performed on the annotated genes. Two significant DMPs annotated to CYP2E1 were found in all samples. In Family One, 1476 DMPs mapped to 880 genes, and 162 DMRs overlapping with 153 unique genes were recognised. Our results suggested that the altered methylation levels of FYN, STAT3, RAC1, and NR4A2 were associated with the development of SZ and ID. Neurodevelopment and the immune system may participate in the occurrence of SZ and ID. Our findings suggested that DNA methylation participated in the development of NDDs by affecting neurodevelopment and the immune system. [ABSTRACT FROM AUTHOR]

Published

2023

16. Exploring risk factors and transmission dynamics of Hepatitis B infection among Indian families: Implications and perspective.

Author

Athalye, Shreyasi, Khargekar, Naveen, Shinde, Shailesh, Parmar, Tejashwini, Chavan, Shreya, Swamidurai, Ganeshmoorthy, Pujari, Vaishali, Panale, Priyanka, Koli, Priyanka, Shankarkumar, Aruna, and Banerjee, Anindita

Abstract

Hepatitis B virus (HBV) is global health problem. Family members of HBV infected people are considered as high-risk groups due to frequent household transmission of HBV among contacts of HBsAg carriers. The present study aimed to investigate the intrafamilial transmission of HBV among family members of HBV-infected persons and to identify the risk factors for viral transmission in these setting. 361 index cases and their 1083 family contacts were tested for markers of Hepatitis B, viz. HBsAg and HBcAb using commercial ELISA. The demographic details and risk factors for acquiring HBV infection among the family members were recorded using a structured questionnaire. The median (IQR) age of index cases and family members was 37 (27 − 48) and 26 (14 − 38) years, respectively. Among the screened family members, 9.23% (n = 100) members were positive for HBsAg and 32.75% (n = 355) were positive for HBcAb. At least one member of the family was affected in 229/361 (63.43%) index cases. Significantly lower percent of household contacts (9.23%, n = 100)were vaccinated against HBV.HBV transmission risk was significantly higher in families with more than four members(p < 0.0001). Multinomial logistics regression analysis for familial risk factors for transmission of HBV such asclose contact with carrier (aOR overt: 1.172, aOR occult: 1.173), sharing of bed/bedding (aOR overt: 1.258, aOR occult:1.264), personal hygiene items (aOR overt:1.260, aOR occult: 1.451), and eating in common utensils (aOR overt: 2.182, aOR occult: 1.307)were significantly associated with the transmission of HBV (p < 0.05). Close contact with carrier, sharing of bed/bedding or personal hygiene items and eating in common utensils were significantly associated with the transmission of HBV. Increasing awareness about Hepatitis B infection and vaccination of family members in close contact with carrier is essential to prevent Hepatitis B transmission. [ABSTRACT FROM AUTHOR]

Published

2023

17. Teoretyczne podstawy towarzyszenia rodzinom zastępczym. W stronę rekomendacji metodycznych z punktu widzenia nauk o rodzinie.

Author

ŻUKIEWICZ, ARKADIUSZ

Abstract

Copyright of Theology & Morality / Teologia I Moralmosc is the property of Uniwersytetu im. Adama Mickiewicza (IH UAM) and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

18. Symptoms of Attenuated Psychosis Syndrome in Relatives of Clinical High-Risk Youth: Preliminary Evidence.

Author

Tarbox-Berry, Sarah I, Walsh, Barbara C, Pogue-Geile, Michael F, and Woods, Scott W

Subjects

SIBLINGS, PSYCHOSES, RISK assessment, COMPARATIVE studies, DESCRIPTIVE statistics, QUESTIONNAIRES, RESEARCH funding, ANXIETY, EARLY diagnosis

Abstract

Background and Hypothesis Attenuated Psychosis Syndrome (APS) impacts functioning and predicts increased risk of psychosis. Risk for developing APS itself has received minimal attention. Knowledge of familial and environmental contributions to APS symptoms would advance understanding of APS and risk for psychosis. As an initial step, this report presents the first data on APS symptoms in family members of APS patients. Study Design This study utilized a discordant sibling-pair family study design. The Structured Interview for Psychosis-risk Syndromes (SIPS) was administered to 17 APS probands and 26 non-APS biological siblings. Probands and siblings were compared on positive, negative, disorganized, and general SIPS symptom scales and factors derived from those scales. Study Results There was significantly greater symptom severity in probands compared to siblings on nine of 19 SIPS scales. Negative/anxiety, functioning, and positive symptom factors were identified. Probands showed significantly greater severity than siblings on the negative/anxiety and positive factors. Elevated pathology on the negative/anxiety factor best differentiated between probands and siblings, over and above the contribution of the positive factor. No difference was found for the functioning factor. Conclusions Results support the importance of non-familial effects on risk for APS and suggest differences in familial contribution to APS symptoms. Understanding the relative contribution of familial and environmental effects on APS symptoms may reveal important differences among APS patients, with implications for risk characterization, symptom course, and treatment selection. [ABSTRACT FROM AUTHOR]

Published

2023

19. Is adult separation anxiety associated with offspring risk for internalizing psychiatric problems?

Author

Finsaas, Megan C. and Klein, Daniel N.

Subjects

*COMPETENCY assessment (Law), *SOCIAL capital, *IMMIGRANTS, *ACCULTURATION, *PSYCHOLOGICAL distress, *KOREAN Americans, *CRONBACH'S alpha, *RESEARCH funding, *SOCIAL cohesion, *QUESTIONNAIRES, *MULTIVARIATE analysis, *SELF medication, *DESCRIPTIVE statistics, *QUALITY of life, *INTERPERSONAL relations, *SOCIODEMOGRAPHIC factors, *COMPARATIVE studies, *OLD age

Abstract

Background: Awareness of adult separation anxiety (ASA) is growing, but there is a dearth of knowledge about how separation anxiety aggregates in families. We examined the intergenerational associations of separation anxiety and other forms of internalizing problems in an American community sample of 515 predominantly white children and their parents. Methods: Children's separation anxiety (CSA), depression, and other anxiety disorders were modeled as latent factors using diagnoses from interviews and symptom scores from questionnaires completed by mothers, fathers, and children when children were 9 years old and again 3 years later. Parents' separation anxiety was assessed via a questionnaire and parents' other anxiety, depressive, and substance use disorders were assessed with a diagnostic interview when children were nine. Relationships between parents' and children's psychopathology were modeled using s.e.m. Results: Mothers' and fathers' ASA were related to all three psychopathology factors in offspring, over and above other parental disorders, in concurrent and prospective analyses. CSA was also related to maternal depression concurrently and prospectively and to maternal anxiety prospectively. Of all paternal psychopathology variables, only ASA was significantly related to children's psychopathology in either model. Conclusions: Results indicate that parental separation anxiety is an important, but non-specific, risk factor for children's psychopathology. The pathway by which this risk is transmitted may be genetic or environmental, and the observed statistical associations likely also encompass child-to-parent effects. [ABSTRACT FROM AUTHOR]

Published

2023

20. A novel deletion mutation accompanied by a point mutation in Lamin A/C gene: Screened from a dilated cardiomyopathy family.

Author

Jia, Hao, Sun, Yongxin, Yao, Wangchao, Chen, Zhenhang, Yang, Shouguo, Wang, Chunsheng, and Lu, Shuyang

Subjects

*GENETIC mutation, *CELL culture, *SEQUENCE analysis, *HUMAN genome, *DILATED cardiomyopathy, *GENES, *GENOMICS, *DESCRIPTIVE statistics, *RESEARCH funding

Abstract

Background: There are 30%–40% of patients with dilated cardiomyopathy (DCM) having genetic causes, among which Lamin A and C gene (LMNA) mutation is the second most frequent DCM-related mutation, and Lamin A/C may be involved in the pathogenesis of DCM through the regulation of gene transcription or the direct effect of cell structure. Methods: Echocardiography and electrocardiogram were used to diagnose DCM and arrhythmia in a DCM family. Then, linked mutations on LMNA were screened out by high-throughput sequencing and verified by Sanger sequencing in all research individuals. Meanwhile, Human Genome Variation Society (HGVS) and Integrative Genomics Viewer (IGV) were used to analyse the characteristics of the mutated Lamin A/C protein. Finally, mutated-type and wild-type LMNA plasmid was transfected into AC-16 cardiomyocytes with the form of a lentivirus vector, and its effect on nucleus and actin was studied by immunofluorescence detection. Results: In this study, we found a new frame-shifted mutation of LMNA (p.Ser414Alafs*66) linked with another point mutation from a DCM family by using High-throughput sequencing, and this deletion mutation led to a truncation of Lamin A/C. By analysing the clinical characteristics of this DCM family, we found that all DCM patients with arrhythmia were carriers of this co-segregation mutation. In the cytological experiment, we found that the mutated-type transfections showed weaker fluorescent intensities on both actin and cell nucleus. Conclusions: A co-segregation mutation of LMNA (Point mutation chr1 156107548 c.1712 G>A and truncated frame-shifted mutation chr1 156106086 c.1240delA) was found from a DCM family, and this type of mutation could participate in the pathogenesis of DCM by affecting the expression of actin. [ABSTRACT FROM AUTHOR]

Published

2023

21. Standing genetic variation affects phenotypic heterogeneity in an SCN5A-mutation founder population with excess sudden cardiac death.

Author

Isaacs, Aaron, Barysenka, Andrei, ter Bekke, Rachel M.A., Helderman-van den Enden, Apollonia T.J.M., van den Wijngaard, Arthur, Volders, Paul G.A., and Stoll, Monika

Abstract

The Worm Study, ascertained from a multigeneration pedigree segregating a single amino acid deletion in SCN5A (c.4850_4852delTCT, p.(Phe1617del), rs749697698), is characterized by substantial phenotypic heterogeneity and overlap of sudden cardiac death, long-QT syndrome, cardiac conduction disease, Brugada syndrome, and isorhythmic atrioventricular dissociation. Linkage analysis for a synthetic trait derived from these phenotypes identified a single peak (logarithm of the odds [LOD] = 4.52) at the SCN5A / SCN10A / SCN11A locus on chromosome 3. This study explored the role of additional genetic variation in the chromosome 3 locus as a source of phenotypic heterogeneity in the Worm Study population. Genotypes underlying the linkage peak (n = 70) were characterized using microarrays. Haplotypes were determined using family-aware phasing and a population-specific reference panel. Variants with minor allele frequencies >0.10 were tested for association with cardiac conduction disease and isorhythmic dissociation using LAMP and logistic regression. Only 1 haplotype carried the p.Phe1617del/rs749697698 deletion, suggesting relatively recent development (∼18 generations); this haplotype contained 5 other missense variants spanning SCN5A / SCN10A / SCN11A. Noncarrier haplotypes (n = 74) ranged in frequency from 0.5% to 5%. Although no variants were associated with cardiac conduction disease, a homozygous missense variant in SCN10A was associated with isorhythmic dissociation after correction for multiple comparisons (odds ratio 11.23; 95% confidence interval 2.76–23.39; P = 1.2 × 10−4). This variant (rs12632942) was previously associated with PR interval. Our data suggest that other variants, alongside a pathogenic mutation, are associated with phenotypic heterogeneity. Single-mutation screening may be insufficient to predict electrical heart disease in patients and family members. In the Worm Study population, segregating a pathogenic SCN5A mutation, compound variation in the SCN5A / SCN10A / SCN11A locus determines arrhythmic outcome. [ABSTRACT FROM AUTHOR]

Published

2023

22. Heritability of apolipoprotein (a) traits in two-generational African-American and Caucasian families[S]

Author

Enkhmaa, Byambaa, Anuurad, Erdembileg, Zhang, Wei, Kim, Kyoungmi, and Berglund, Lars

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Clinical Research, Minority Health, Adolescent, Adult, Black or African American, Aged, Alleles, Apoprotein(a), Child, Female, Genetic Variation, Humans, Inheritance Patterns, Male, Middle Aged, White People, Young Adult, lipoprotein, apolipoprotein (a) isoform, LPA allele, heritability estimates, family resemblance, family study, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

Heritability of LPA allele, apo(a) isoform sizes, and isoform-associated lipoprotein(a) [Lp(a)] levels was studied in 82 Caucasian and African-American families with two parents and two children (age: 6-74 years). We determined: 1) Lp(a) levels; 2) LPA allele sizes; 3) apo(a) isoform sizes; and 4) isoform-specific apo(a) levels (ISLs), the amount of Lp(a) carried by an individual apo(a) isoform. Trait heritability was estimated by mid-parent-offspring analysis. The ethnicity-adjusted heritability estimate for Lp(a) level was 0.95. Heritability for ISLs corresponding to the smaller LPA allele in a given allele-pair was higher than that corresponding to the larger LPA allele (0.91 vs. 0.59, P = 0.017). Although not statistically different, heritability for both apo(a) isoforms (0.90 vs. 0.70) and LPA alleles (0.98 vs. 0.82) was higher for the smaller versus larger sizes. Heritability was generally lower in African-Americans versus Caucasians with a 4-fold difference for the larger LPA allele (0.25 vs. 0.94, P = 0.001). In Caucasians, an overall higher heritability pattern was noted for the older (≥47 years) versus younger (

Published

2019

23. Coronary Artery Disease Risk and Lipidomic Profiles Are Similar in Hyperlipidemias With Family History and Population‐Ascertained Hyperlipidemias

Author

Rämö, Joel T, Ripatti, Pietari, Tabassum, Rubina, Söderlund, Sanni, Matikainen, Niina, Gerl, Mathias J, Klose, Christian, Surma, Michal A, Stitziel, Nathan O, Havulinna, Aki S, Pirinen, Matti, Salomaa, Veikko, Freimer, Nelson B, Jauhiainen, Matti, Palotie, Aarno, Taskinen, Marja‐Riitta, Simons, Kai, and Ripatti, Samuli

Subjects

Atherosclerosis, Digestive Diseases, Heart Disease, Cardiovascular, Aetiology, 2.1 Biological and endogenous factors, Adult, Cholesterol, LDL, Coronary Artery Disease, Family, Female, Finland, Humans, Hypercholesterolemia, Hyperlipidemias, Hypertriglyceridemia, Lipidomics, Male, Medical History Taking, Middle Aged, Proportional Hazards Models, Triglycerides, coronary artery disease, family study, high-risk populations, hypercholesterolemia, hypertriglyceridemia, lipids and lipoproteins, high‐risk populations, Cardiorespiratory Medicine and Haematology

Abstract

Background We asked whether, after excluding familial hypercholesterolemia, individuals with high low-density lipoprotein cholesterol ( LDL -C) or triacylglyceride levels and a family history of the same hyperlipidemia have greater coronary artery disease risk or different lipidomic profiles compared with population-based hyperlipidemias. Methods and Results We determined incident coronary artery disease risk for 755 members of 66 hyperlipidemic families (≥2 first-degree relatives with similar hyperlipidemia) and 19 644 Finnish FINRISK population study participants. We quantified 151 circulating lipid species from 550 members of 73 hyperlipidemic families and 897 FINRISK participants using mass spectrometric shotgun lipidomics. Familial hypercholesterolemia was excluded using functional LDL receptor testing and genotyping. Hyperlipidemias ( LDL -C or triacylglycerides >90th population percentile) associated with increased coronary artery disease risk in meta-analysis of the hyperlipidemic families and the population cohort (high LDL -C: hazard ratio, 1.74 [95% CI, 1.48-2.04]; high triacylglycerides: hazard ratio, 1.38 [95% CI, 1.09-1.74]). Risk estimates were similar in the family and population cohorts also after adjusting for lipid-lowering medication. In lipidomic profiling, high LDL -C associated with 108 lipid species, and high triacylglycerides associated with 131 lipid species in either cohort (at 5% false discovery rate; P-value range 0.038-2.3×10-56). Lipidomic profiles were highly similar for hyperlipidemic individuals in the families and the population ( LDL -C: r=0.80; triacylglycerides: r=0.96; no lipid species deviated between the cohorts). Conclusions Hyperlipidemias with family history conferred similar coronary artery disease risk as population-based hyperlipidemias. We identified distinct lipidomic profiles associated with high LDL -C and triacylglycerides. Lipidomic profiles were similar between hyperlipidemias with family history and population-ascertained hyperlipidemias, providing evidence of similar and overlapping underlying mechanisms.

Published

2019

24. A Comprehensive Genetic Analysis of Slovenian Families with Multiple Cases of Orofacial Clefts Reveals Novel Variants in the Genes IRF6 , GRHL3 , and TBX22.

Author

Slavec, Lara, Geršak, Ksenija, Eberlinc, Andreja, Hovnik, Tinka, Lovrečić, Luca, Mlinarič-Raščan, Irena, and Karas Kuželički, Nataša

Subjects

*GENETIC variation, *COMPARATIVE genomic hybridization, *GENE families, *CLEFT palate, *SYMPTOMS, *FRAMESHIFT mutation

Abstract

Although the aetiology of non-syndromic orofacial clefts (nsOFCs) is usually multifactorial, syndromic OFCs (syOFCs) are often caused by single mutations in known genes. Some syndromes, e.g., Van der Woude syndrome (VWS1; VWS2) and X-linked cleft palate with or without ankyloglossia (CPX), show only minor clinical signs in addition to OFC and are sometimes difficult to differentiate from nsOFCs. We recruited 34 Slovenian multi-case families with apparent nsOFCs (isolated OFCs or OFCs with minor additional facial signs). First, we examined IRF6, GRHL3, and TBX22 by Sanger or whole exome sequencing to identify VWS and CPX families. Next, we examined 72 additional nsOFC genes in the remaining families. Variant validation and co-segregation analysis were performed for each identified variant using Sanger sequencing, real-time quantitative PCR and microarray-based comparative genomic hybridization. We identified six disease-causing variants (three novel) in IRF6, GRHL3, and TBX22 in 21% of families with apparent nsOFCs, suggesting that our sequencing approach is useful for distinguishing syOFCs from nsOFCs. The novel variants, a frameshift variant in exon 7 of IRF6, a splice-altering variant in GRHL3, and a deletion of the coding exons of TBX22, indicate VWS1, VWS2, and CPX, respectively. We also identified five rare variants in nsOFC genes in families without VWS or CPX, but they could not be conclusively linked to nsOFC. [ABSTRACT FROM AUTHOR]

Published

2023

25. Examining the Construct Validity of Borderline Personality Traits Using Familial Aggregation and Other External Validators.

Author

Letkiewicz, Allison M., Spring, Justin D., Carrillo, Vivian L., and Shankman, Stewart A.

Subjects

*RESEARCH methodology evaluation, *BORDERLINE personality disorder, *MULTITRAIT multimethod techniques, *DISEASE susceptibility, *DESCRIPTIVE statistics, *QUESTIONNAIRES, *DATA analysis software

Abstract

Numerous studies have questioned the reliability and validity of borderline personality disorder's (BPD) categorical conceptualization. DSM-5 Section III's alternative trait-based model of BPD may better capture borderline pathology, but aspects of its validity should be further established. Thus, the authors examined whether a latent BPD factor derived from Section III traits exhibits (1) familial aggregation among siblings and (2) association with constructs related to borderline pathology. The authors also tested whether gender moderated associations. A total of 498 community-recruited adults completed the Personality Inventory for DSM-5, a behavioral assessment of risk-taking, and reported their history of childhood maltreatment, substance use, nonsuicidal self-injury, and suicidal ideation. Familial aggregation was assessed among 232 sibling pairs. Siblings' BPD scores were significantly correlated and most external validators were significantly associated with BPD, with the exception of risk-taking. Results did not vary by gender. Findings further support the construct validity of Section III's BPD trait profile. [ABSTRACT FROM AUTHOR]

Published

2022

26. Family-based whole-exome sequencing implicates a variant in lysyl oxidase like 4 in atypical femur fractures.

Author

Zhou W, van de Laarschot DM, van Rooij JGJ, Koedam M, Nguyen HH, Uitterlinden AG, Ebeling PR, Thakker RV, Geusens P, van der Eerden BCJ, Verkerk AJMH, and Zillikens MC

Subjects

Humans, Female, Male, Aged, Amino Acid Oxidoreductases genetics, Middle Aged, Osteoblasts metabolism, Osteoblasts pathology, Protein-Lysine 6-Oxidase, Exome Sequencing, Femoral Fractures genetics, Femoral Fractures pathology, Pedigree

Abstract

Atypical femur fractures (AFFs) are rare adverse events associated with bisphosphonate use, having unclear pathophysiology. AFFs also cluster in families and have occurred in patients with monogenetic bone diseases sometimes without bisphosphonate use, suggesting an underlying genetic susceptibility. Our aim was to identify a genetic cause for AFF in a Caucasian family with 7 members affected by osteoporosis, including 3 siblings with bisphosphonate-associated AFFs. Using whole-exome sequencing, we identified a rare pathogenic variant c.G1063A (p.Gly355Ser) in lysyl oxidase like 4 (LOXL4) among 64 heterozygous rare, protein-altering variants shared by the 3 siblings with AFFs. The same variant was also found in a fourth sibling with a low-trauma femur fracture above the knee, not fulfilling all the ASBMR criteria of AFF and in 1 of 73 unrelated European AFF patients. LOXL4 is involved in collagen cross-linking and may be relevant for microcrack formation and bone repair mechanisms. Preliminary functional analysis showed that skin fibroblast-derived osteoblasts from the unrelated patient with the LOXL4 variant expressed less collagen type I and elastin, while osteogenic differentiation and mineralization were enhanced compared with 2 controls. In conclusion, this LOXL4 variant may underlie AFF susceptibility possibly due to abnormal collagen metabolism, leading to increased formation of microdamage or compromised healing of microcracks in the femur., (© The Author(s) 2024. Published by Oxford University Press on behalf of the American Society for Bone and Mineral Research.)

Published

2024

27. Genetic Understanding of Obsessive-Compulsive Disorder and Related Disorders

Author

Samuels, Jack and Tolin, David F., book editor

Published

2023

28. Familial risk of postpartum depression.

Author

Rasmussen, Marie‐Louise H., Poulsen, Gry J., Wohlfahrt, Jan, Videbech, Poul, and Melbye, Mads

Subjects

*POSTPARTUM depression, *FAMILY history (Medicine), *MENTAL illness, *ANTIDEPRESSANTS

Abstract

Objective: Many psychiatric diseases have a strong familial aggregation, but it is unknown whether postpartum depression (PPD) without prior psychiatric history aggregates in families. Methods: Based on Danish national registers, we constructed a cohort with information on 848,544 singleton deliveries (1996–2017). Women with an episode of PPD were defined as having used antidepressant medication and/or had a hospital contact for depression within 6 months after delivery. Those with psychiatric history prior to the delivery were excluded. We estimated relative risk (RR) of PPD, comparing women with female relatives with and without PPD history, respectively. Results: Overall, women with a PPD history in female blood relatives had themselves a higher risk of PPD (RR = 1.64, 95% CI 1.16–2.34). Having the first‐degree female relative with PPD history was associated with a more than 2.5 times (RR = 2.65, 95% CI 1.79–3.91) increased risk of PPD. However, having the second/third‐degree female relative and/or a female non‐blood relative with PPD history did not increase the woman's own risk of PPD (RR = 0.58, 95% CI 0.26–1.28, RR = 1.09, 95% CI 0.83–1.44). Conclusion: Postpartum depression aggregates in families with no other psychiatric history, but the findings do not support a strong genetic trait as a major cause. Other possible mechanisms are shared environment and/or health‐seeking behavior in close relationships. [ABSTRACT FROM AUTHOR]

Published

2022

29. The associations of parental COVID‐19 related worries, lifestyles, and insomnia with child insomnia during the COVID‐19 outbreak.

Author

Zhan, Nalan, Zhang, Yeqing, Xie, Dongjie, and Geng, Fulei

Subjects

*COVID-19 pandemic, *SCREEN time, *PARENT-child relationships, *INSOMNIA, *COVID-19, *PRESCHOOL children, *UNCERTAINTY

Abstract

The impacts of the Coronavirus Disease 2019 (COVID‐19) pandemic on sleep health have been studied extensively. However, little is known about sleep problems within the family system during the pandemic. This study aimed to examine the influence of the COVID‐19 pandemic on insomnia in both adults and children, and to explore whether parental COVID‐19 related worries, lifestyles, and insomnia were associated with child insomnia. A total of 1355 parent–child dyads (39.2% fathers, mean age 38.37 years, SD = 5.34; 52.7% boys, mean age 12.47 years, SD = 1.67) were recruited from Jiangxi province in China from 4 to 18 February 2020. Data on insomnia, COVID‐19 related worries, physical activity, and screen time were collected using online questionnaires. Path analysis showed that COVID‐19 related worries and screen time were positively associated with insomnia in both parents and children; while children's physical activity was negatively related to children's insomnia. Parents' insomnia, COVID‐19 related worries, physical activity, and screen time were positively associated with children's insomnia, COVID‐19 related worries, physical activity, and screen time, respectively. Bootstrap tests showed that parents' worries were positively associated with children's insomnia via parents' insomnia and children's worries; parents' physical activity was negatively associated with children's insomnia via children's physical activity, parents' screen time was positively associated with children's insomnia via parents' insomnia and children's screen time. Both parental and child sleep are affected by the pandemic. Parental insomnia, stress reaction, and lifestyles contribute to child insomnia. Child sleep health may be maintained or improved by family bonds, home exercise, and sleep schedules. [ABSTRACT FROM AUTHOR]

Published

2022

30. Case Report: Aarskog-scott syndrome caused by FGD1 gene variation: A family study.

Author

Yijia Liang, Honglin Wu, Xiumei He, and Xiyu He

Subjects

GENE families, PHENOTYPIC plasticity, GENETIC variation, SYNDROMES, GENETIC disorders

Abstract

Aarskog-Scott syndrome is a rare genetic disorder characterized by short stature, abnormal facial features, and digital and genital deformities. FGD1 gene variation is the known cause of this disorder. This paper described a Chinese family study of Aarskog-Scott syndrome in which the main patients were two brothers. Then, the relationship between genotype and phenotype in Aarskog-Scott syndrome was investigated preliminarily. A new FGD1 gene variant was revealed in this study, providing insights into the link between phenotype and genotype variations in Aarskog-Scott syndrome as well as a foundation for its diagnosis and treatment. [ABSTRACT FROM AUTHOR]

Published

2022

31. Whole Exome Sequencing in Two Southeast Asian Families With Atypical Femur Fractures.

Author

Zhou, Wei, Nguyen, Hanh H., van de Laarschot, Denise M., Howe, Tet Sen, Koh, Joyce S.B., Milat, Frances, van Rooij, Jeroen G.J., Verlouw, Joost A.M., van der Eerden, Bram C.J., Stevenson, Mark, Thakker, Rajesh V., Zillikens, M. Carola, and Ebeling, Peter R.

Subjects

FEMORAL fractures, GENETIC variation, FAMILIES, THERAPEUTIC complications, FAMILIAL spastic paraplegia

Abstract

Atypical femur fractures (AFFs) are rare complications of anti‐resorptive therapy. Devastating to the affected individual, they pose a public health concern because of reduced uptake of an effective treatment for osteoporosis due to patient concern. The risk of AFF is increased sixfold to sevenfold in patients of Asian ethnicity compared with Europeans. Genetic factors may underlie the AFF phenotype. Given the rarity of AFFs, studying familial AFF cases is valuable in providing insights into any genetic predisposition. We present two Singaporean families, one comprising a mother (1‐a) and a daughter (1‐b), and the other comprising two sisters (2‐a and 2‐b). All four cases presented with bisphosphonate‐associated AFF. Whole‐exome sequencing (WES) was performed on 1‐b, 2‐a, and 2‐b. DNA for 1‐a was not available. Variants were examined using a candidate gene approach comprising a list of genes previously associated with AFF in the literature, as well as using unbiased filtering based on dominant and/or recessive inheritance patterns. Using a candidate gene approach, rare variants shared between all three cases were not identified. A rare variant in TMEM25, shared by the two sisters (2‐a and 2‐b), was identified. A rare heterozygous PLOD2 variant was present in the daughter case with AFF (1‐b), but not in the sisters. A list of potential genetic variants for AFF was identified after variant filtering and annotation analysis of the two sisters (2‐a and 2‐b), including a Gly35Arg variant in TRAF4, a gene required for normal skeletal development. Although the findings from this genetic analysis are inconclusive, a familial aggregation of AFFs is suggestive of a genetic component in AFF pathogenesis. We provide a comprehensive list of rare variants identified in these AFF familial cases to aid future genetic studies. © 2022 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research. [ABSTRACT FROM AUTHOR]

Published

2022

32. Whole Exome Sequencing in Two Southeast Asian Families With Atypical Femur Fractures

Author

Wei Zhou, Hanh H. Nguyen, Denise M. van deLaarschot, Tet Sen Howe, Joyce S.B. Koh, Frances Milat, Jeroen G.J. van Rooij, Joost A.M. Verlouw, Bram C.J. van der Eerden, Mark Stevenson, Rajesh V. Thakker, M. Carola Zillikens, and Peter R. Ebeling

Subjects

ATYPICAL FEMUR FRACTURE, BISPHOSPHONATES, FAMILY STUDY, GENES, OSTEOPOROSIS, Orthopedic surgery, RD701-811, Diseases of the musculoskeletal system, RC925-935

Abstract

ABSTRACT Atypical femur fractures (AFFs) are rare complications of anti‐resorptive therapy. Devastating to the affected individual, they pose a public health concern because of reduced uptake of an effective treatment for osteoporosis due to patient concern. The risk of AFF is increased sixfold to sevenfold in patients of Asian ethnicity compared with Europeans. Genetic factors may underlie the AFF phenotype. Given the rarity of AFFs, studying familial AFF cases is valuable in providing insights into any genetic predisposition. We present two Singaporean families, one comprising a mother (1‐a) and a daughter (1‐b), and the other comprising two sisters (2‐a and 2‐b). All four cases presented with bisphosphonate‐associated AFF. Whole‐exome sequencing (WES) was performed on 1‐b, 2‐a, and 2‐b. DNA for 1‐a was not available. Variants were examined using a candidate gene approach comprising a list of genes previously associated with AFF in the literature, as well as using unbiased filtering based on dominant and/or recessive inheritance patterns. Using a candidate gene approach, rare variants shared between all three cases were not identified. A rare variant in TMEM25, shared by the two sisters (2‐a and 2‐b), was identified. A rare heterozygous PLOD2 variant was present in the daughter case with AFF (1‐b), but not in the sisters. A list of potential genetic variants for AFF was identified after variant filtering and annotation analysis of the two sisters (2‐a and 2‐b), including a Gly35Arg variant in TRAF4, a gene required for normal skeletal development. Although the findings from this genetic analysis are inconclusive, a familial aggregation of AFFs is suggestive of a genetic component in AFF pathogenesis. We provide a comprehensive list of rare variants identified in these AFF familial cases to aid future genetic studies. © 2022 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.

Published

2022

33. Executive functioning in adults with borderline personality disorder and first-degree biological relatives.

Author

Koudys, Jacob W. and Ruocco, Anthony C.

Subjects

*EXECUTIVE function, *BORDERLINE personality disorder, *FISHER discriminant analysis, *RESPONSE inhibition, *COGNITIVE flexibility

Abstract

Behavioural dysregulation is a heritable core symptom domain in borderline personality disorder (BPD) that is likely influenced by the integrity of executive functions (EFs). However, the extent to which familial risk for BPD confers decrement to EFs has yet to be comprehensively studied. In this family study, probands with BPD (n = 73), first-degree biological relatives (n = 65), and healthy controls without psychiatric diagnoses (n = 77) were assessed in abstraction, attentional vigilance, working memory, cognitive flexibility, interference resolution, planning, problem solving, and response inhibition. In univariate analyses, probands demonstrated lower response inhibition than relatives. Comparatively, discriminant function analyses revealed that lower interference resolution and response inhibition jointly discriminated probands from relatives and controls, whereas a combination of less efficient problem solving and difficulty manipulating mental information discriminated probands and relatives from controls. Moreover, the subset of psychiatrically non-affected relatives demonstrated a pattern of resilience to psychiatric morbidity substantiated by stronger response inhibition and abstraction abilities despite less efficient problem solving. Familial risk for BPD is represented predominantly by a pattern of problem-solving and working memory deficits. Resilience to a psychiatric disorder in non-affected relatives reflects both EF weaknesses and strengths, highlighting potential protective factors that should be considered in future neurocognitive research on BPD families. [ABSTRACT FROM AUTHOR]

Published

2022

34. A Series of 14 Polish Patients with Thrombotic Events and PC Deficiency-Novel c.401-1G>A PROC Gene Splice Site Mutation in a Patient with Aneurysms.

Author

Weronska, Anna, Potaczek, Daniel P., Oto, Julia, Medina, Pilar, Undas, Anetta, and Wypasek, Ewa

Subjects

*GENETIC engineering, *MISSENSE mutation, *VENOUS thrombosis, *ANEURYSMS, *PROTEIN C, *GENETIC mutation

Abstract

Objectives: Protein C (PC) deficiency is an inherited thrombophilia with a prevalence of 0.5% in the general population and 3% in subjects with a first-time deep vein thrombosis (DVT). Here we report a series of 14 PC-deficient Polish patients with comprehensive clinical and molecular characteristics, including long-term follow-up data and a deep mutational analysis of the PROC gene. Patients and Methods: Fourteen unrelated probands (mean ± SD age 43.8 ± 13.0 years) with suspicion of PC deficiency, who experienced thromboembolic events and a majority of whom received anticoagulants (92.8%), were screened for PROC mutations by sequencing the nine PROC exons and their flanking intron regions. Results: Ten probands (71.4%) had missense mutations, two patients (14.3%) carried nonsense variants, and the other two subjects (14.3%) had splice-site mutations, the latter including the c.401-1G>A variant, reported here for the very first time. The proband carrying the c.401-1A allele had a hepatic artery aneurysm with a highly positive family history of aneurysms and the absence of any mutations known to predispose to this vascular anomaly. Conclusion: A novel detrimental PROC mutation was identified in a family with aneurysms, which might suggest yet unclear links of thrombophilia to vascular anomalies, including aneurysms at atypical locations in women. The present case series also supports data indicating that novel oral anticoagulants (NOACs) are effective in PC deficient patients. [ABSTRACT FROM AUTHOR]

Published

2022

35. Subjectivity and respect for fundamental rights in professional child care practice. Review article

Author

Żukiewicz, Arkadiusz and Żukiewicz, Arkadiusz

Abstract

This article is the result of the analysis of the content of a scientific monograph. In the course of the analysis, the desc-research method was used. The aim of the research was to present to Polish readers an up-to-date and cognitively interesting foreign scientific monograph. This book fits into the field of family study (family pedagogy, etc.). The background to further polemics is the presentation of issues raised by the authors of individual monograph chapters–these concerns mainly concern childcare activities, protecting children’s rights, and active participation in society. The summary shows the substantive value of the monograph and its practical (methodical) values, which can be an inspiration for further research conducted in the fields of research and theoretical and useful activity., Artykuł powstał na podstawie analizy treści monografii naukowej. Zastosowano metodę desc-research. Celem podjętych badań była prezentacja polskim czytelnikom aktualnej i poznawczo interesującej, zagranicznej monografii naukowej. Publikacja ta wpisuje się w pole nauk o rodzinie (pedagogiki rodziny itp.). Tłem wprowadzającym do dalszej polemiki są nakreślone zagadnienia, podjęte przez autorów poszczególnych rozdziałów monografii. Dotyczą one w szczególności obszarów odnoszących się do praktyki działalności opiekuńczej nad dziećmi oraz ochrony praw dzieci i ich aktywnego udziału w życiu społecznym. W podsumowaniu zaprezentowano merytoryczną wartość monografii oraz jej walory praktyczne (metodyczne), które mogą stanowić inspirację w toku kolejnych poszukiwań, prowadzonych na polach aktywności badawczej, teoretycznej oraz praktycznej.

Published

2024

36. Mood disorders as a risk factor for family aggregation of somatic diseases

Author

E. Kasyanov and G. Mazo

Subjects

Depression, somatic diseases, family study, bipolar disorder, Psychiatry, RC435-571

Abstract

Introduction Mood disorders (MDs) are associated with somatic diseases and tend to aggregate in families. But there are limited studies on the risk of somatic diseases for relatives of patients with MDs. Objectives To assess whether a patient’s mood disorder diagnosis is associated with a family history of somatic disorders. Methods This cross-sectional family study included 36 patients with MDs (66.7% women; age - 32 [11.2] years) and 68 of their relatives, and 23 healthy individuals (56,5% women; age - 30.5 [6.9] years) and 53 of their relatives. A Pearson’s χ2 test was used to compare the frequencies of family history of somatic disease. Logistic regression models were used to determine the independent association of MDs, after adjusting for the effects of sex, age, with binary characteristics. Results Individuals with and without MDs had different frequencies of family history of cardiovascular (66,7% vs. 43,4%; p=0,03) and endocrinological diseases (47,2% vs. 39,1%; p=0,04). There were no statistically significant differences in the frequency of family history of gastrointestinal, pulmonary, urogenital and musculoskeletal diseases (p>0,05). Logistic regression revealed that MDs diagnosis in patients was a risk factor for cardiovascular (p=0.03, OR=3.5) and endocrinological disease (p=0.04, OR=3.7) in their relatives. Conclusions MDs are associated with the aggregation of somatic diseases in families. Future research is needed to clarify the biological reasons for this association. Disclosure No significant relationships.

Published

2022

37. Burden of Type 2 Diabetes and Associated Cardiometabolic Traits and Their Heritability Estimates in Endogamous Ethnic Groups of India: Findings From the INDIGENIUS Consortium.

Author

Venkatesan, Vettriselvi, Lopez-Alvarenga, Juan Carlos, Arya, Rector, Ramu, Deepika, Koshy, Teena, Ravichandran, Umarani, Ponnala, Amaresh Reddy, Sharma, Surendra K., Lodha, Sailesh, Sharma, Krishna K., Shaik, Mahaboob Vali, Resendez, Roy G., Venugopal, Priyanka, R, Parthasarathy, Saju, Noelta, Ezeilo, Juliet A., Bejar, Cynthia, Wander, Gurpreet S., Ralhan, Sarju, and Singh, Jai Rup

Subjects

TYPE 2 diabetes, ETHNIC groups, HERITABILITY, GENETIC profile, BLOOD pressure

Abstract

To assess the burden of type 2 diabetes (T2D) and its genetic profile in endogamous populations of India given the paucity of data, we aimed to determine the prevalence of T2D and estimate its heritability using family-based cohorts from three distinct Endogamous Ethnic Groups (EEGs) representing Northern (Rajasthan [Agarwals: AG]) and Southern (Tamil Nadu [Chettiars: CH] and Andhra Pradesh [Reddys: RE]) states of India. For comparison, family-based data collected previously from another North Indian Punjabi Sikh (SI) EEG was used. In addition, we examined various T2D-related cardiometabolic traits and determined their heritabilities. These studies were conducted as part of the Indian Diabetes Genetic Studies in collaboration with US (INDIGENIUS) Consortium. The pedigree, demographic, phenotypic, covariate data and samples were collected from the CH, AG, and RE EEGs. The status of T2D was defined by ADA guidelines (fasting glucose ≥ 126 mg/dl or HbA1c ≥ 6.5% and/or use of diabetes medication/history). The prevalence of T2D in CH (N = 517, families = 21, mean age = 47y, mean BMI = 27), AG (N = 530, Families = 25, mean age = 43y, mean BMI = 27), and RE (N = 500, Families = 22, mean age = 46y, mean BMI = 27) was found to be 33%, 37%, and 36%, respectively, Also, the study participants from these EEGs were found to be at increased cardiometabolic risk (e.g., obesity and prediabetes). Similar characteristics for the SI EEG (N = 1,260, Families = 324, Age = 51y, BMI = 27, T2D = 75%) were obtained previously. We used the variance components approach to carry out genetic analyses after adjusting for covariate effects. The heritability (h2) estimates of T2D in the CH, RE, SI, and AG were found to be 30%, 46%, 54%, and 82% respectively, and statistically significant (P ≤ 0.05). Other T2D related traits (e.g., BMI, lipids, blood pressure) in AG, CH, and RE EEGs exhibited strong additive genetic influences (h2 range: 17% [triglycerides/AG and hs-CRP/RE] - 86% [glucose/non-T2D/AG]). Our findings highlight the high burden of T2D in Indian EEGs with significant and differential additive genetic influences on T2D and related traits. [ABSTRACT FROM AUTHOR]

Published

2022

38. Perceived Physical Fatigability Predicts All-Cause Mortality in Older Adults.

Author

Glynn, Nancy W, Gmelin, Theresa, Renner, Sharon W, Qiao, Yujia (Susanna), Boudreau, Robert M, Feitosa, Mary F, Wojczynski, Mary K, Cosentino, Stephanie, Andersen, Stacy L, Christensen, Kaare, and Newman, Anne B

Subjects

*OLDER people, *MORTALITY, *PROPORTIONAL hazards models, *LONGEVITY, *PHYSICAL diagnosis, *AGING, *RESEARCH funding, *FATIGUE (Physiology)

Abstract

Background: Perceived physical fatigability is highly prevalent in older adults and associated with mobility decline and other health consequences. We examined the prognostic value of perceived physical fatigability as an independent predictor of risk of death among older adults.Methods: Participants (N = 2 906), mean age 73.5 [SD, 10.4] years, 54.2% women, 99.7% white enrolled in the Long Life Family Study, were assessed at Visit 2 (2014-2017) with 2.7 [SD, 1.0] years follow-up. The Pittsburgh Fatigability Scale (PFS), a 10-item, self-administered validated questionnaire (score range 0-50, higher = greater fatigability) measured perceived physical fatigability at Visit 2. Deaths post-Visit 2 through December 31, 2019 were identified by family members notifying field centers, reporting during another family member's annual phone follow-up, an obituary, or Civil Registration System (Denmark). We censored all other participants at their last contact. Cox proportional hazard models predicted mortality by fatigability severity, adjusted for family relatedness and other covariates.Results: Age-adjusted PFS Physical scores were higher for those who died (19.1 [SE, 0.8]) compared with alive (12.2, [SE, 0.4]) overall, as well as across age strata (p < .001), except for those 60-69 years (p = .79). Participants with the most severe fatigability (PFS Physical scores ≥ 25) were over twice as likely to die (hazard ratio, 2.33 [95% CI, 1.65-3.28]) compared with those who had less severe fatigability (PFS Physical scores < 25) after adjustment.Conclusions: Our work underscores the utility of the PFS as a novel patient-reported prognostic indicator of phenotypic aging that captures both overt and underlying disease burden that predicts death. [ABSTRACT FROM AUTHOR]

Published

2022

39. No association between the Ser9Gly polymorphism of the dopamine receptor D3 gene and schizophrenia: a meta-analysis of family-based association studies

Author

Xiao-na Li, Ji-long Zheng, Xiao-han Wei, Bao-jie Wang, and Jun Yao

Subjects

Dopamine receptor D3, Schizophrenia, Meta-analysis, Family study, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Previous studies found that Ser9Gly (rs6280) might be involved in the occurrence of schizophrenia. However, no consist conclusion has yet been achieved. Compared to the case-control study, the family-based study took into account stratification bias. Thus, we conducted a meta-analysis of family-based studies to measure a pooled effect size of the association between Ser9Gly and the risk of schizophrenia. Methods The relevant family-based studies were screened using the electronic databases by the inclusion criteria. Odds ratios (ORs) and 95% confidence intervals (CIs) were used to measure the correction between Ser9Gly polymorphism and schizophrenia susceptibility. Subgroup analysis was performed by stratification of ethnicity (i.e., East Asian, Caucasian, and other populations). Additionally, publication bias was evaluated by the funnel plot. Results After literature searching, a total of 13 family-based association studies were included, which contained 11 transmission disequilibrium test (TDT) studies with 1219 informative meiosis and 5 haplotype-based haplotype relative risk (HRR) studies. No statistical significance of the heterogeneity was detected in TDT and HRR studies. Thus, the pooled effect size was calculated under the fixed effect model. The results found that the association was significantly protective in East Asian in TDT studies (204 informative meiosis, OR = 0.744, 95% CI = 0.564–0.980, Z-value = − 2.104, p = 0.035). Conclusions The meta-analysis based on the family study found a protective association of Ser9Gly in East Asian. In future, large sample molecular epidemiology studies are needed to validate our findings.

Published

2020

40. Quantitative trait variation in ASD probands and toddler sibling outcomes at 24 months

Author

Jessica B. Girault, Meghan R. Swanson, Shoba S. Meera, Rebecca L. Grzadzinski, Mark D. Shen, Catherine A. Burrows, Jason J. Wolff, Juhi Pandey, Tanya St John, Annette Estes, Lonnie Zwaigenbaum, Kelly N. Botteron, Heather C. Hazlett, Stephen R. Dager, Robert T. Schultz, John N. Constantino, Joseph Piven, and for the IBIS Network

Subjects

Autism, Infant sibling, Family study, Language, Communication, Development, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract Background Younger siblings of children with autism spectrum disorder (ASD) are at increased likelihood of receiving an ASD diagnosis and exhibiting other developmental concerns. It is unknown how quantitative variation in ASD traits and broader developmental domains in older siblings with ASD (probands) may inform outcomes in their younger siblings. Methods Participants included 385 pairs of toddler siblings and probands from the Infant Brain Imaging Study. ASD probands (mean age 5.5 years, range 1.7 to 15.5 years) were phenotyped using the Autism Diagnostic Interview-Revised (ADI-R), the Social Communication Questionnaire (SCQ), and the Vineland Adaptive Behavior Scales, Second Edition (VABS-II). Siblings were assessed using the ADI-R, VABS-II, Mullen Scales of Early Learning (MSEL), and Autism Diagnostic Observation Schedule (ADOS) and received a clinical best estimate diagnosis at 24 months using DSM-IV-TR criteria (n = 89 concordant for ASD; n = 296 discordant). We addressed two aims: (1) to determine whether proband characteristics are predictive of recurrence in siblings and (2) to assess associations between proband traits and sibling dimensional outcomes at 24 months. Results Regarding recurrence risk, proband SCQ scores were found to significantly predict sibling 24-month diagnostic outcome (OR for a 1-point increase in SCQ = 1.06; 95% CI = 1.01, 1.12). Regarding quantitative trait associations, we found no significant correlations in ASD traits among proband-sibling pairs. However, quantitative variation in proband adaptive behavior, communication, and expressive and receptive language was significantly associated with sibling outcomes in the same domains; proband scores explained 9–18% of the variation in cognition and behavior in siblings with ASD. Receptive language was particularly strongly associated in concordant pairs (ICC = 0.50, p

Published

2020

41. Low Risk for Developing Diabetes Among the Offspring of Individuals With Exceptional Longevity and Their Spouses

Author

Iva Miljkovic, Ryan Cvejkus, Ping An, Bharat Thyagarajan, Kaare Christensen, Mary Wojczynski, Nicole Schupf, and Joseph M. Zmuda

Subjects

diabetes, longevity, offspring, long-living individuals, Family Study, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Little is known about the risk of type 2 diabetes (T2D) among the offspring of individuals with exceptional longevity. We determined the incidence of and potential risk and protective factors for T2D among the offspring of probands and offspring’s spouses (mean age=60 years, range 32-88 years) in the Long Life Family Study (LLFS), a multicenter cohort study of 583 two-generation families with a clustering of healthy aging and exceptional longevity. Incident T2D was defined as fasting serum glucose ≥126 mg/dl, or HbA1c of ≥6.5%, or self-reported with doctor diagnosis of T2D, or the use of anti-diabetic medication during a mean follow-up 7.9 ± 1.1 years. Among offspring (n=1105) and spouses (n=328) aged 45-64 years without T2D at baseline visit, the annual incident rate of T2D was 3.6 and 3.0 per 1000 person-years, respectively, while among offspring (n=444) and spouses (n=153) aged 65+ years without T2D at baseline, the annual incident rate of T2D was 7.2 and 7.4 per 1000 person-years, respectively. By comparison, the annual incident rate of T2D per 1000 person-years in the U.S. general population was 9.9 among those aged 45-64, and 8.8 among those aged 65+ years (2018 National Health Interview Survey). Baseline BMI, waist circumference, and fasting serum triglycerides were positively associated with incident T2D, whereas fasting serum HDL-C, adiponectin, and sex hormone binding globulin were protective against incident T2D among the offspring (all P

Published

2022

42. Burden of Type 2 Diabetes and Associated Cardiometabolic Traits and Their Heritability Estimates in Endogamous Ethnic Groups of India: Findings From the INDIGENIUS Consortium

Author

Vettriselvi Venkatesan, Juan Carlos Lopez-Alvarenga, Rector Arya, Deepika Ramu, Teena Koshy, Umarani Ravichandran, Amaresh Reddy Ponnala, Surendra K. Sharma, Sailesh Lodha, Krishna K. Sharma, Mahaboob Vali Shaik, Roy G. Resendez, Priyanka Venugopal, Parthasarathy R, Noelta Saju, Juliet A. Ezeilo, Cynthia Bejar, Gurpreet S. Wander, Sarju Ralhan, Jai Rup Singh, Narinder K. Mehra, Raghavendra Rao Vadlamudi, Marcio Almeida, Srinivas Mummidi, Chidambaram Natesan, John Blangero, Krishna M. Medicherla, Sadagopan Thanikachalam, Thyagarajan Sadras Panchatcharam, Dileep Kumar Kandregula, Rajeev Gupta, Dharambir K. Sanghera, Ravindranath Duggirala, and Solomon F. D. Paul

Subjects

type 2 diabetes, cardiometabolic traits, Indian population, epidemiology, genetic epidemiology, family study, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

To assess the burden of type 2 diabetes (T2D) and its genetic profile in endogamous populations of India given the paucity of data, we aimed to determine the prevalence of T2D and estimate its heritability using family-based cohorts from three distinct Endogamous Ethnic Groups (EEGs) representing Northern (Rajasthan [Agarwals: AG]) and Southern (Tamil Nadu [Chettiars: CH] and Andhra Pradesh [Reddys: RE]) states of India. For comparison, family-based data collected previously from another North Indian Punjabi Sikh (SI) EEG was used. In addition, we examined various T2D-related cardiometabolic traits and determined their heritabilities. These studies were conducted as part of the Indian Diabetes Genetic Studies in collaboration with US (INDIGENIUS) Consortium. The pedigree, demographic, phenotypic, covariate data and samples were collected from the CH, AG, and RE EEGs. The status of T2D was defined by ADA guidelines (fasting glucose ≥ 126 mg/dl or HbA1c ≥ 6.5% and/or use of diabetes medication/history). The prevalence of T2D in CH (N = 517, families = 21, mean age = 47y, mean BMI = 27), AG (N = 530, Families = 25, mean age = 43y, mean BMI = 27), and RE (N = 500, Families = 22, mean age = 46y, mean BMI = 27) was found to be 33%, 37%, and 36%, respectively, Also, the study participants from these EEGs were found to be at increased cardiometabolic risk (e.g., obesity and prediabetes). Similar characteristics for the SI EEG (N = 1,260, Families = 324, Age = 51y, BMI = 27, T2D = 75%) were obtained previously. We used the variance components approach to carry out genetic analyses after adjusting for covariate effects. The heritability (h2) estimates of T2D in the CH, RE, SI, and AG were found to be 30%, 46%, 54%, and 82% respectively, and statistically significant (P ≤ 0.05). Other T2D related traits (e.g., BMI, lipids, blood pressure) in AG, CH, and RE EEGs exhibited strong additive genetic influences (h2 range: 17% [triglycerides/AG and hs-CRP/RE] - 86% [glucose/non-T2D/AG]). Our findings highlight the high burden of T2D in Indian EEGs with significant and differential additive genetic influences on T2D and related traits.

Published

2022

43. Cohort profile and representativeness of participants in the Diet, Cancer and Health—Next Generations cohort study.

Author

Petersen, Kristina E. N., Halkjær, Jytte, Loft, Steffen, Tjønneland, Anne, and Olsen, Anja

Subjects

COHORT analysis, DIET, FAMILIES, SOCIOECONOMIC factors, BIOMATERIALS

Abstract

The Diet, Cancer and Health—Next Generations (DCH-NG) study is a large population-based cohort study that was established as a resource for transgenerational research. The cohort is an extension of the Diet, Cancer and Health (DCH) cohort. The aim of this paper was to describe the study design and methods and to investigate the representativeness of participants by comparing participants with non-participants with emphasis on socioeconomic determinants. In 2015–2019, children (G1), their spouses (G1P) and grandchildren (G2) of DCH cohort members were invited to participate. Participants completed questionnaires, a physical examination and collection of biological material. Information on general and sociodemographic variables was obtained by linkage to administrative registries in Denmark. The cohort includes 39,554 adult participants with complete data collection. Participants are represented in different family structures including 2- and 3-generation relationships, offspring-parents trios and siblings. The odds ratio for participation was highest among G1, females, middle-aged and married individuals and individuals with the highest education, highest income, occupations requiring high-level skills and residency near a study centre. The different family structures allow a range of studies with cohort and transgenerational designs. The pattern of more likelihood of participation in higher socioeconomic groups was similar to the pattern of participation in the DCH cohort and the general patterns in population-based studies. Accordingly, the study population has some limitations as to being representative of the general population. Yet, the DCH-NG cohort will provide valuable insight on the association between risk factor-disease relationships and the role of heredity on these associations. [ABSTRACT FROM AUTHOR]

Published

2022

44. Genetic analysis of four consanguineous multiplex families with inflammatory bowel disease.

Author

Ben-Yosef, Noam, Frampton, Matthew, Schiff, Elena R, Daher, Saleh, Baker, Fadi Abu, Safadi, Rifaat, Israeli, Eran, Segal, Anthony W, and Levine, Adam P

Abstract

Background Family studies support a genetic predisposition to inflammatory bowel diseases (IBD), but known genetic variants only partially explain the disease heritability. Families with multiple affected individuals potentially harbour rare and high-impact causal variants. Long regions of homozygosity due to recent inbreeding may increase the risk of individuals bearing homozygous loss-of-function variants. This study aimed to identify rare and homozygous genetic variants contributing to IBD. Methods Four families with known consanguinity and multiple cases of IBD were recruited. In a family-specific analysis, we utilised homozygosity mapping complemented by whole-exome sequencing. Results We detected a single region of homozygosity shared by Crohn's disease cases from a family of Druze ancestry, spanning 2.6 Mb containing the NOD2 gene. Whole-exome sequencing did not identify any potentially damaging variants within the region, suggesting that non-coding variation may be involved. In addition, affected individuals in the families harboured several rare and potentially damaging homozygous variants in genes with a role in autophagy and innate immunity including LRRK1 , WHAMM , DENND3 , and C5. Conclusion This study examined the potential contribution of rare, high-impact homozygous variants in consanguineous families with IBD. While the analysis was not designed to achieve statistical significance, our findings highlight genes or loci that warrant further research. Non-coding variants affecting NOD2 may be of importance in Druze patients with Crohn's disease. [ABSTRACT FROM AUTHOR]

Published

2021

45. Identification of Pathogenic CNVs in Unexplained Developmental Disabilities Using Exome Sequencing: A Family Trio Study.

Author

Naumova, O. Yu., Dobrynin, P. V., Gibitova, E. A., Zhukova, M. A., Rychkov, S. Yu., Zhukova, O. V., and Grigorenko, E. L.

Subjects

*DEVELOPMENTAL disabilities, *DNA copy number variations, *DEVELOPMENTAL delay, *FISHING techniques, *FAMILIES

Abstract

This short report on a family case-study provides evidence of the effectiveness of exome sequencing of family trios (proband-parents) as the first-tier test in genomic diagnostics of unexplained developmental delays and disorders, as a genomic screening for both pathogenic single-nucleotide variants and copy number variations (CNVs). In this study, we identified several clinically significant de novo structural genomic variations in the proband's genome, specifically those associated with the 17p11.2 duplication (or Potocki–Lupski) syndrome. These genome rearrangements were externally confirmed by certified clinical laboratories using both FISH and MLPA techniques. [ABSTRACT FROM AUTHOR]

Published

2021

46. Rate of Heart Failure Following Atrial Fibrillation According to Presence of Family History of Dilated Cardiomyopathy or Heart Failure: A Nationwide Study

Author

Magnus N. Ebbesen, Maria D’Souza, Charlotte Andersson, Jawad H. Butt, Christian Madelaire, Tor Biering‐Sorensen, Morten Lock‐Hansen, Soren Lund Kristensen, Gunnar Gislason, Lars Kober, Christian Torp‐Pedersen, and Morten Schou

Subjects

atrial fibrillation heart failure, family history, family study, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background It is poorly understood why some patients with atrial fibrillation develop heart failure (HF) and others do not. We examined the rate of developing HF in patients with atrial fibrillation with and without first‐degree family members with HF or dilated cardiomyopathy (DCM). Methods and Results Using Danish nationwide registries, patients born after 1942 diagnosed with atrial fibrillation in the period 2005 to 2015 were identified and followed for up to 5 years. Patients with pre‐existing HF, DCM, and/or ischemic heart disease diagnoses were excluded. Exposure was defined as a first‐degree relative with HF or DCM. The rate of developing the composite end point of HF or death, and the components, was estimated with multivariable Cox proportional hazard regression models. We included 10 605 patients. A total of 17% had a family member with DCM/HF. Having a family member with HF/DCM was associated with an increased 5‐year risk of the composite of HF/death (cumulative incidence, 9.2% [95% CI, 7.8–10.7] versus 5.6% [95% CI, 5.0–6.1]; adjusted hazard ratio [HR] 1.36 [95% CI, 1.13–1.64]). (HF 8.4% [95% CI, 7.0–9.8] versus 4.5% [95% CI, 4.1–5.0]); (adjusted HR, 1.49 [95% CI, 1.22–1.82]). However, familial HF/DCM was not significantly associated with an increased 5‐year risk and rate of death (0.8% [95% CI, 0.4–1.2] versus 1.1% [95% CI, 0.8–1.3]); (adjusted HR, 0.80 [95% CI, 0.46–1.39]). Conclusions In patients with incident atrial fibrillation without prior ischemic heart disease or HF diagnoses, 1 of 6 had a first‐degree relative with HF, and having such a family history of HF/DCM was associated with an 87% increase in 5‐year incidence of HF compared with those without.

Published

2021

47. Is processing speed a valid neurocognitive endophenotype in bipolar disorder? Evidence from a longitudinal, family study.

Author

Luperdi, Sussy C., Correa-Ghisays, Patricia, Vila-Francés, Joan, Selva-Vera, Gabriel, Salazar-Fraile, José, Cardoner, Narcís, Ruiz-Veguilla, Miguel, Livianos, Lorenzo, Tabarés-Seisdedos, Rafael, and Balanzá-Martínez, Vicent

Subjects

*BIPOLAR disorder, *SPEED, *SYMPTOMS, *FAMILIES

Abstract

Substantial evidence supports the existence of neurocognitive endophenotypes in bipolar disorder (BD), but very few longitudinal studies have included unaffected relatives. In a 5-year, follow-up, family study, we have recently suggested that deficits in manual motor speed and visual memory could be endophenotype candidates for BD. We aimed to explore whether this also applies to processing speed. A sample of 348 individuals, including 163 BD patients, 65 unaffected first-degree relatives (BD-Rel) and 120 genetically unrelated healthy controls (HC), was assessed with the Digit Symbol Substitution Test (DSST) on two occasions over a 2-year period (T1, T2). DSST values were controlled for age, years of education, occupational status, and subsyndromic mood symptoms. Differences between groups were evaluated with ANCOVAs. At T1 BD performed significantly worse than HC (p < 0.001; Cohen's d = 1.38) and BD-Rel (p < 0.001; Cohen's d = 0.82). BD-Rel showed an intermediate performance with significant differences with HC (p < 0.01; Cohen's d = 0.50). Similarly, at T2 BD performed significantly worse than HC (p < 0.001; Cohen's d = 1.44) and BD-Rel (p < 0.01; Cohen's d = 0.51). BD-Rel performance was intermediate and significantly lower than that of HC (p < 0.01; Cohen's d = 0.97). A Repeated Measures ANOVA revealed no significant between-group differences in performance over time (p > 0.05). The results of this longitudinal, family study suggest that impaired processing speed may represent a suitable cognitive endophenotype for BD. Further research on the field is required to confirm these preliminary findings. • The endophenotypic nature of processing speed in bipolar disorder is uncertain. • Longitudinal family studies may be a suitable strategy for its identification. • Both patients and unaffected relatives showed a persistent deficit. • Impaired processing speed may be a valid endophenotype of bipolar disorder. [ABSTRACT FROM AUTHOR]

Published

2021

48. Heritability of apolipoprotein (a) traits in two-generational African-American and Caucasian families[S]

Author

Byambaa Enkhmaa, Erdembileg Anuurad, Wei Zhang, Kyoungmi Kim, and Lars Berglund

Subjects

lipoprotein (a), apolipoprotein (a) isoform, LPA allele, heritability estimates, family resemblance, family study, Biochemistry, QD415-436

Abstract

Heritability of LPA allele, apo(a) isoform sizes, and isoform-associated lipoprotein(a) [Lp(a)] levels was studied in 82 Caucasian and African-American families with two parents and two children (age: 6–74 years). We determined: 1) Lp(a) levels; 2) LPA allele sizes; 3) apo(a) isoform sizes; and 4) isoform-specific apo(a) levels (ISLs), the amount of Lp(a) carried by an individual apo(a) isoform. Trait heritability was estimated by mid-parent-offspring analysis. The ethnicity-adjusted heritability estimate for Lp(a) level was 0.95. Heritability for ISLs corresponding to the smaller LPA allele in a given allele-pair was higher than that corresponding to the larger LPA allele (0.91 vs. 0.59, P = 0.017). Although not statistically different, heritability for both apo(a) isoforms (0.90 vs. 0.70) and LPA alleles (0.98 vs. 0.82) was higher for the smaller versus larger sizes. Heritability was generally lower in African-Americans versus Caucasians with a 4-fold difference for the larger LPA allele (0.25 vs. 0.94, P = 0.001). In Caucasians, an overall higher heritability pattern was noted for the older (≥47 years) versus younger (

Published

2019

49. Arrhythmogenic cardiomyopathy with left ventricular involvement versus ischemic heart disease: lessons learned from the family study and the reviewed autopsy of a young male

Author

Pilar Molina, Jorge Sanz-Sánchez, Manuel Fenollosa, Marina Martínez-Matilla, Juan Giner, and Esther Zorio

Subjects

forensic sciences, forensic pathology, ischemic heart disease, arrhythmogenic cardiomyopathy, family study, Criminal law and procedure, K5000-5582, Public aspects of medicine, RA1-1270

Abstract

Ischemic heart disease (IHD) is the leading cause of sudden cardiac death (SCD) and often non-thrombosed severe coronary stenoses with or without myocardial scars are detected. Left dominant arrhythmogenic cardiomyopathy (LDAC) is a life-threating rare disease which has been more thoroughly studied in the last 10 years. The macroscopic study of an SCD victim was conducted and re-evaluated 9 years later. The cardiological work-up in his first-degree relatives initially comprised an electrocardiogram (ECG) and an echocardiogram. When they were re-evaluted 9 years later, a cardiac magnetic resonance, an ECG-monitoring, an exercise testing and a genetic study were performed and the pedigree was extended accordingly. In 2008, an IHD was suspected in the sports-triggered SCD of a 37-year-old man upon the postmortem (75% stenosis of the left main and circumflex coronary arteries; the subepicardial left ventricular fibrofatty infiltration with mild myocardial degeneration was assumed to be a past myocardial infarction). No cardiomyopathy was identified in any of the two proband’s sisters. Nine years thereafter, distant relatives were diagnosed with LDAC due to a pathogenic desmoplakin mutation. The reanalysis of the two sisters showed ventricular arrhythmias in one of them without structural heart involvement and the reviewed postmortem of the proband was reclassified as LDAC based on the fibrofatty infiltration; both were mutation carriers. The completion of the family study on 19 family members yielded one SCD due to LDAC (the proband), three living patients diagnosed with LDAC (two with a defibrillator), one mutation carrier without structural ventricular involvement, and 14 healthy relatives (who were discharged) with a very good co-segregation of the mutation. Although rare, LDAC exists and sometimes its differential diagnosis with IHD has to be faced. Modifying previous postmortem misdiagnoses can help family screening to further prevent SCDs.

Published

2019

50. Standing genetic variation affects phenotypic heterogeneity in an SCN5A-mutation founder population with excess sudden cardiac death

Author

Aaron Isaacs, Andrei Barysenka, Rachel M.A. ter Bekke, Apollonia T.J.M. Helderman-van den Enden, Arthur van den Wijngaard, Paul G.A. Volders, and Monika Stoll

Subjects

SELECTION, RISK, R-PACKAGE, LOCI, COMMON VARIANTS, ASSOCIATION, Family study, DISEASE, Ventricular tachyarrhythmia, Cardiac conduction disease, Modifier genes, Standing genetic variation, Physiology (medical), LINKAGE, INTERVAL, Isorhythmic atrioventricular dissociation, Com-pound variation, Cardiology and Cardiovascular Medicine

Abstract

Background: The Worm Study, ascertained from a multigeneration pedigree segregating a single amino acid deletion in SCN5A (c.4850_4852delTCT, p.(Phe1617del), rs749697698), is characterized by substantial phenotypic heterogeneity and overlap of sudden cardiac death, long-QT syndrome, cardiac conduction disease, Brugada syndrome, and isorhythmic atrioventricular dissociation. Linkage analysis for a synthetic trait derived from these phenotypes identified a single peak (logarithm of the odds [LOD] = 4.52) at the SCN5A/SCN10A/SCN11A locus on chromosome 3. Objective: This study explored the role of additional genetic variation in the chromosome 3 locus as a source of phenotypic heterogeneity in the Worm Study population. Methods: Genotypes underlying the linkage peak (n = 70) were characterized using microarrays. Haplotypes were determined using family-aware phasing and a population-specific reference panel. Variants with minor allele frequencies >0.10 were tested for association with cardiac conduction disease and isorhythmic dissociation using LAMP and logistic regression. Results: Only 1 haplotype carried the p.Phe1617del/rs749697698 deletion, suggesting relatively recent development (∼18 generations); this haplotype contained 5 other missense variants spanning SCN5A/SCN10A/SCN11A. Noncarrier haplotypes (n = 74) ranged in frequency from 0.5% to 5%. Although no variants were associated with cardiac conduction disease, a homozygous missense variant in SCN10A was associated with isorhythmic dissociation after correction for multiple comparisons (odds ratio 11.23; 95% confidence interval 2.76–23.39; P = 1.2 × 10 −4). This variant (rs12632942) was previously associated with PR interval. Conclusion: Our data suggest that other variants, alongside a pathogenic mutation, are associated with phenotypic heterogeneity. Single-mutation screening may be insufficient to predict electrical heart disease in patients and family members. In the Worm Study population, segregating a pathogenic SCN5A mutation, compound variation in the SCN5A/SCN10A/SCN11A locus determines arrhythmic outcome.

Published

2023