Your search keyword '"Cannon-Albright L"' showing total 27 results

1. The contribution of the rs55705857 G allele to familial cancer risk as estimated in the Utah population database.

Author

Hummel S, Kohlmann W, Kollmeyer TM, Jenkins R, Sonnen J, Palmer CA, Colman H, Abbott D, Cannon-Albright L, and Cohen AL

Subjects

Alleles, Astrocytoma genetics, Databases, Factual, Family, Female, Genetic Predisposition to Disease, Homozygote, Humans, Information Storage and Retrieval, Isocitrate Dehydrogenase genetics, Male, Mutation, Neoplasms genetics, Oligodendroglioma genetics, Utah, Brain Neoplasms genetics, Chromosomes, Human, Pair 8 genetics, Colorectal Neoplasms genetics, Germ-Line Mutation genetics, Glioma genetics, Prostatic Neoplasms genetics, Thyroid Neoplasms genetics

Abstract

Background: IDH1/2 mutated glioma has been associated with a germline risk variant, the rs55705857 G allele. The Utah Population Database (UPDB), a computerized genealogy of people in Utah, is a unique resource to evaluate cancer risk in related individuals., Methods: One hundred and two individuals with IDH1/2 mutant or 1p/19q co-deleted glioma were genotyped and linked to the UPDB. DNA came from blood (21), tumor tissue (43), or both (38). We determined congruence between somatic and germline samples and estimated the relative risk for developing cancer to first and second-degree relatives of G and A allele carriers at rs55705857., Results: Somatic (glioma) DNA had 85.7% sensitivity (CI 57.2-98.2%) and 95.8% specificity (CI 78.9-99.89%) for germline rs55705857 G allele. Forty-one patients were linked to pedigrees in the UPDB with at least three generations of data. First-degree relatives of rs55705857 G allele carriers were at significantly increased risk for developing cancer (RR = 1.72, p = 0.045, CI 1.02-2.94), and specifically for oligodendroglioma (RR = 57.61, p = 0.017, CI 2.96-320.98) or prostate cancer (RR = 4.10, p = 0.008, CI 1.62-9.58); relatives of individuals without the G allele were not at increased risk. Second-degree relatives of G allele carriers also had significantly increased risk for developing cancer (RR = 1.50, p = 0.007, CI 1.15-2.01)., Conclusions: Tumor DNA may approximate genotype at the rs55705857 locus. We confirmed this locus confers an increased risk of all cancers and especially of oligodendroglioma. No increased cancer or brain tumor risk is seen in family members of individuals without the high-risk G allele.

Published

2019

2. Risk of associated conditions in relatives of subjects with interstitial cystitis.

Author

Allen-Brady K, Norton PA, and Cannon-Albright L

Subjects

Comorbidity, Constipation epidemiology, Cystitis, Interstitial epidemiology, Female, Fibromyalgia epidemiology, Humans, Male, Myalgia epidemiology, Myositis epidemiology, Myositis genetics, Pedigree, Risk, Utah epidemiology, Constipation genetics, Cystitis, Interstitial genetics, Family, Fibromyalgia genetics, Genetic Predisposition to Disease, Myalgia genetics

Abstract

Objectives: Urological chronic pelvic pain syndrome includes interstitial cystitis/painful bladder syndrome (IC/PBS), a chronic bladder pain condition of unknown etiology. Interstitial cystitis/painful bladder syndrome can co-occur with a number of associated conditions such as irritable bowel syndrome and fibromyalgia. The purpose of this study was to estimate the heritability of approximately 20 associated conditions in first-degree relatives (and if appropriate, second- and third-degree relatives) of patients with IC/PBS to identify shared genetic contributions for the disease combinations., Methods: We used the Utah Population Database, a unique population-based genealogical database that has been linked to electronic health records for the University of Utah Health Sciences Center back in 1994. Interstitial cystitis/painful bladder syndrome probands were identified by the International Classification of Diseases, Ninth Revision code for chronic interstitial cystitis and had genealogy information for 12 of their 14 immediate ancestors. We calculated excess risk of an associated condition in relatives of patients with IC/PBS using relative risk estimates., Results: We identified 248 IC/PBS probands. We found that 2 associated conditions, myalgia and myositis/unspecified (fibromyalgia) as well as constipation, were in significant excess in the patients with IC/PBS themselves, their first-degree relatives, and their second-degree relatives. The excess risk among relatives between IC/PBS and these associated conditions also held in the converse direction. Excess risk of IC/PBS was observed in the first- and second-degree relatives in probands with myalgia and myositis/unspecified (fibromyalgia) and in probands with constipation., Conclusions: These results suggest that myalgia and myositis/unspecified (fibromyalgia) as well as constipation are likely to share underlying genetic factors with IC/PBS.

Published

2015

3. Familial clustering of ALS in a population-based resource.

Author

Gibson SB, Figueroa KP, Bromberg MB, Pulst SM, and Cannon-Albright L

Subjects

Aged, Cluster Analysis, Cohort Studies, Female, Humans, Male, Middle Aged, Utah epidemiology, Amyotrophic Lateral Sclerosis diagnosis, Amyotrophic Lateral Sclerosis epidemiology, Amyotrophic Lateral Sclerosis genetics, Databases, Factual trends, Population Surveillance methods

Abstract

Objective: To determine the extent of an inherited contribution to amyotrophic lateral sclerosis (ALS) mortality., Methods: Death certificates (DCs) from 1904 to 2009 were analyzed from patients with at least 3 generations recorded in the Utah Population Database, a genealogic and medical database of more than 2 million Utah residents. Among probands whose DCs listed ALS, the relative risk (RR) of death with ALS was determined among spouses and first- through fifth-degree relatives, using birth year-, sex-, and birthplace-matched cohorts., Results: Eight hundred seventy-three patients with ALS met the inclusion criteria. Among 3,531 deceased first-degree relatives of probands, the RR of dying with ALS was increased compared with control cohorts (RR = 4.91, 95% confidence interval 3.36, 6.94). The RR of dying with ALS was also increased among 9,386 deceased second-degree relatives (RR = 2.85, 95% confidence interval 2.06, 3.84). The RR of dying with ALS was not increased among third- through fifth-degree relatives. More affected first-degree relatives were male (p = 0.014). No cases of conjugal ALS were observed., Conclusions: This study is suggestive of familial clustering in excess of expected for ALS. Our results confirm the results of prior studies of familial ALS, suggesting applicability of our findings to other mixed European populations. Furthermore, this work expands on previous studies by quantifying the RR of ALS among more distant relatives. The use of mortality data obtained from DCs reduces the ascertainment and recall bias of many previous studies. Finally, the excess of ALS among second-degree relatives and lack of conjugal ALS are strongly supportive of a genetic contribution.

Published

2014

4. Use of a genealogical database demonstrates heritability of pulmonary fibrosis.

Author

Scholand MB, Coon H, Wolff R, and Cannon-Albright L

Subjects

Death Certificates, Female, Genetic Predisposition to Disease genetics, Humans, Male, Pedigree, Pulmonary Fibrosis mortality, Retrospective Studies, Risk Factors, Utah, Databases, Factual statistics & numerical data, Genealogy and Heraldry, Pulmonary Fibrosis epidemiology, Pulmonary Fibrosis genetics

Abstract

Background: Pulmonary fibrosis (PF) is a progressive fatal disease of unknown etiology. Identification of risk genes and pathways will enhance our understanding of this disease. Analysis of Utah genealogical resources has shown previously strong evidence for a genetic contribution to other disease, such as cancer. This approach has led to gene discovery in diseases, such as breast cancer and colon cancer and is used here for PF to quantify the heritability., Hypothesis: We hypothesize that there is a heritable contribution to death from PF and use existing genealogic and death certificate data to examine patterns of relatedness amongst individuals who have died of PF., Methods: We analyzed familial clustering of individuals who died from PF using the Utah Population Database, a unique population-based genealogical resource that has been linked to death certificates dating from 1904. We identified 1,000 individuals with at least three generations of genealogy data and a cause of death documented as PF (cases). We estimated the relative risk (RR) of death from PF among the first-, second-, and third-degree relatives of cases. We also tested the hypothesis of excess relatedness among the cases by comparing the average pairwise relatedness of all cases to the average pair-wise relatedness of 1,000 sets of matched controls., Results: We observed significantly increased risk for death from PF among the first- (RR = 4.69), second- (RR = 1.92), and third-degree relatives (RR = 1.14) of cases. The average relatedness of the 1,000 cases was significantly higher than the expected average relatedness of matched control sets (p < 0.001). When close (first- and second-degree) relationships were ignored, significantly increased relatedness remained (p = 0.002)., Conclusions: Our results demonstrate significant clustering among both close and distant relatives, providing strong support for genetic contributions to death from PF. High-risk pedigrees derived from this unique resource may help identify new risk genes and gene pathways.

Published

2013

5. A unique genome-wide association analysis in extended Utah high-risk pedigrees identifies a novel melanoma risk variant on chromosome arm 10q.

Author

Teerlink C, Farnham J, Allen-Brady K, Camp NJ, Thomas A, Leachman S, and Cannon-Albright L

Subjects

Case-Control Studies, Female, Genotype, Humans, Linkage Disequilibrium, Male, Pedigree, Risk Factors, Utah, Chromosomes, Human, Pair 10 genetics, Genetic Predisposition to Disease, Genome-Wide Association Study, Melanoma genetics, Polymorphism, Single Nucleotide genetics

Abstract

Only two genome-wide association (GWA) screens have been published for melanoma (Nat Genet 47:920-925, 2009; Nat Genet 40:838-840, 2008). Using a unique approach, we performed a genome-wide association study in 156 related melanoma cases from 34 high-risk Utah pedigrees. Genome-wide association analysis was performed on nearly 500,000 markers; we compared cases to 2,150 genotypically matched samples from Illumina's iControls database. We performed genome-wide association with EMMAX software, which is designed to account for population structure, including relatedness between cases. Three SNPs exceeded a genome-wide significance threshold of p < 5 × 10(-8) on chromosome arm 10q25.1 (rs17119434, rs17119461, and rs17119490), where the most extreme p value was 7.21 × 10(-12). This study represents a new and unique approach to predisposition gene identification; and it is the first genome-wide association study performed in related cases in high-risk pedigrees. Our approach illustrates an example of using high-risk pedigrees for the identification of new melanoma predisposition variants.

Published

2012

6. Identification of six loci associated with pelvic organ prolapse using genome-wide association analysis.

Author

Allen-Brady K, Cannon-Albright L, Farnham JM, Teerlink C, Vierhout ME, van Kempen LCL, Kluivers KB, and Norton PA

Subjects

Adult, Aged, Aged, 80 and over, Case-Control Studies, Female, Gene Frequency, Genome, Human, Humans, Middle Aged, Netherlands, Utah, White People, Young Adult, Pelvic Organ Prolapse genetics, Polymorphism, Single Nucleotide

Abstract

Objective: There is evidence that both environmental and genetic factors contribute to pelvic organ prolapse. We conducted a genome-wide association study to investigate whether common genetic variants modify the risk of pelvic organ prolapse., Methods: We recruited women who had been evaluated and treated for pelvic organ prolapse at the University of Utah from 1996 to 2008 and their affected female relatives. Those in the case group were genotyped on the Illumina 550K platform. We genetically matched 2,976 white control participants available from Illumina as the control group. Association tests were adjusted for related participants using two different software programs: EMMAX and Genie. Confirmation of findings was performed in a cohort of Dutch women (n=76) with recurrent pelvic organ prolapse and family history of pelvic organ prolapse., Results: The Utah study sample included 115 case group participants treated for pelvic organ prolapse, in most case group participants with surgery (n=78) or repeat surgery (n=35). Results from association analyses using EMMAX software identified five single-nucleotide polymorphisms (SNPs) significantly associated with pelvic organ prolapse (P<1×10). Independent association analysis with Genie software identified three of the same SNPs and one additional SNP. The six SNPs were located at 4q21 (rs1455311), 8q24 (rs1036819), 9q22 (rs430794), 15q11 (rs8027714), 20p13 (rs1810636), and 21q22 (rs2236479). Nominally significant findings (P<.05) or findings trending toward significance (P<.1) were observed for five of the six SNPs in the Dutch cohort., Conclusion: Six SNPs have been identified that are significantly associated with pelvic organ prolapse in high-risk familial case group participants and that provide evidence for a genetic contribution to pelvic organ prolapse., Level of Evidence: II.

Published

2011

7. Parapneumonic empyema deaths during past century, Utah.

Author

Bender JM, Ampofo K, Sheng X, Pavia AT, Cannon-Albright L, and Byington CL

Subjects

Adolescent, Adult, Child, Disease Outbreaks history, Disease Outbreaks statistics & numerical data, Empyema, Pleural epidemiology, History, 20th Century, History, 21st Century, Humans, Infant, Influenza, Human complications, Influenza, Human epidemiology, Influenza, Human mortality, Pneumonia, Bacterial mortality, Pneumonia, Pneumococcal mortality, Utah epidemiology, Empyema, Pleural history, Empyema, Pleural mortality, Influenza, Human history, Pneumonia, Bacterial history, Pneumonia, Pneumococcal history

Abstract

Bacterial pneumonia with empyema is a serious complication of influenza and commonly resulted in death during the 1918 influenza pandemic. We hypothesize that deaths caused by parapneumonic empyema are increasing in Utah once again despite advances in critical care and the availability of antimicrobial drugs and new vaccines. In this study, we analyzed the historical relationship between deaths caused by empyema and influenza pandemics by using 100 years of data from Utah. Deaths caused by empyema have indeed increased from 2000-2004 when compared with the historic low death rates of 1950-1975. Vaccine strategies and antimicrobial drug stockpiling to control empyema will be important as we prepare for the next influenza pandemic.

Published

2009

8. Enabling GeneHunter as a grid service: a case study for implementing analytical services for biomedical grids.

Author

Krikov S, Price RC, Allen-Brady K, Cannon-Albright L, and Facelli JC

Subjects

Utah, Chromosome Mapping methods, Computational Biology methods, Internet, Software, User-Computer Interface

Abstract

Advances in grid computing show promise for easier provisioning of analytical services to biomedical researchers. In this poster we present our experiences in creating a grid analytical service based on the popular genetic linkage analysis tool GeneHunter. We have implemented and deployed this grid service using tools available from the caGrid project. Our results show that caGrid tools are quite effective and compare favorably with other existing methodologies.

Published

2008

9. Familiality of diabetes mellitus.

Author

Weires MB, Tausch B, Haug PJ, Edwards CQ, Wetter T, and Cannon-Albright LA

Subjects

Adolescent, Adult, Aged, Databases, Factual, Family, Female, Humans, Male, Middle Aged, Pedigree, Risk, Risk Factors, Utah, Diabetes Mellitus, Type 1 genetics, Diabetes Mellitus, Type 2 genetics

Abstract

The aims of this study were to estimate relative risk for type 1 and type 2 diabetes in relatives of diabetic patients, and to test for excess relatedness among diabetic patients. Additionally, the difference in parental transmission of diabetes was investigated. This study used a unique Utah genealogical resource, linked to electronic medical records of the largest health provider in Utah. We identified 19,640 patients with a diagnosis of type 1 or type 2 diabetes. Relative Risks (RRs) for type 1 and type 2 diabetes were assessed for first-, second- and third-degree relatives of diabetic patients. The observed average relatedness of diabetic patients was compared to the expected relatedness using the Genealogical Index of Familiality (GIF). We observed significantly elevated RRs for type 1 diabetes in first-degree (RR=8.68; P<0.0001), second-degree (RR=1.93; P<0.0001) and third-degree relatives (RR=1.74; P<0.0001) of type 1 diabetic patients. RRs for type 2 diabetes were significantly increased in first-degree (RR=2.24; P<0.0001), second-degree (RR=1.36; P<0.0001) and third-degree relatives (RR=1.14; P<0.0001) of type 2 diabetic patients. Significantly increased RRs for type 1 diabetes were observed in the relatives of type 2 diabetic patients, and vice versa. The GIF analysis showed significant excess relatedness for type 1 diabetes cases, and independently for type 2 diabetes cases. Offspring of diabetic fathers were at significantly higher risk for type 1 diabetes than offspring of diabetic mothers (RR=9.73; P<0.0001 compared to RR=4.99; P<0.0001). No significant difference in parental transmission was observed for type 2 diabetes. Our results strongly support the existence of a genetic contribution to both type 1 and type 2 diabetes, and additionally suggest a relationship between both types of diabetes. Furthermore, our results suggest a significant difference in parental transmission of type 1 diabetes.

Published

2007

10. Genome-wide linkage analysis for aggressive prostate cancer in Utah high-risk pedigrees.

Author

Christensen GB, Camp NJ, Farnham JM, and Cannon-Albright LA

Subjects

Aged, DNA, Neoplasm analysis, Genotype, Humans, Lod Score, Male, Microsatellite Repeats, Middle Aged, Pedigree, Prostatic Neoplasms epidemiology, Utah epidemiology, Genetic Linkage, Genetic Predisposition to Disease, Genome, Human, Prostatic Neoplasms genetics

Abstract

Background: It has been proposed that studying alternative phenotypes, such as tumor aggressiveness, may be a solution for overcoming the apparent heterogeneity that has hindered the identification of prostate cancer (PC) genes. We present the results of a genome-scan for predisposition to aggressive PC using the Utah high-risk pedigree resource., Methods: We identified 259 subjects with aggressive PC in 57 extended and nuclear families. Parametric and non-parametric multipoint linkage statistics were calculated for a genome-wide set of 401 microsatellite markers using the MCLINK software package. Stratification analyses by the number of affected subjects per pedigree (<5, >or=5) and the average age at diagnosis of affected subjects (<70 years, >or=70 years) were also performed., Results: No significant results were observed at the genome-wide level, but suggestive evidence for linkage was observed on chromosomes 9q (HLOD = 2.04) and 14q (HLOD = 2.08); several pedigrees showed individual evidence for linkage at each locus (LOD > 0.58). The subset of pedigrees with earlier age at onset demonstrated nominal linkage evidence on chromosomes 3q (HLOD = 1.79), 8q (HLOD = 1.67), and 20q (HLOD=1.82). The late-onset subset showed suggestive linkage on chromosome 6p (HLOD = 2.37) and the subset of pedigrees with fewer than five affected subjects showed suggestive linkage on chromosome 10p (HLOD = 1.99)., Conclusions: Linkage evidence observed on chromosomes 6p, 8q, and 20q support previously reported PC aggressiveness loci. While these results are encouraging, further research is necessary to identify the gene or genes responsible for PC aggressiveness and surmount the overarching problem of PC heterogeneity., ((c) 2007 Wiley-Liss, Inc.)

Published

2007

11. A population-based assessment of the familial component of chronic kidney disease mortality.

Author

Goldfarb-Rumyantzev AS, Cheung AK, Habib AN, Wang BJ, Lin SJ, Baird BC, Naiman N, and Cannon-Albright L

Subjects

Cause of Death, Databases, Genetic, Death Certificates, Evaluation Studies as Topic, Genetic Predisposition to Disease epidemiology, Humans, Kidney Failure, Chronic epidemiology, Registries, Risk Factors, Utah epidemiology, Genealogy and Heraldry, Kidney Failure, Chronic genetics, Kidney Failure, Chronic mortality, Pedigree, Population

Abstract

Background/aim: While the familial nature of chronic kidney disease (CKD) has been recognized, it has primarily been defined from studies of first-degree relatives of selected sets of cases. The goal of this study is an evaluation of the familial clustering of end-stage renal disease (ESRD) and CKD mortality using a population-based genealogy of Utah. This is the first population-based analysis of the familial component of ESRD and non-ESRD CKD., Methods: We have defined two distinct patient groups for this analysis, using individuals with death certificates in the Utah Population Database indicating ESRD (n = 192) and non-ESRD CKD (n = 335) as the cause of death. Two measures of familiality were used: (1) relative risk (RR) of CKD or ESRD death in relatives of cases and (2) an average relatedness statistic, i.e., the Genealogical Index of Familiality., Results: The RR for dying with ESRD among the first-degree relatives of individuals dying with ESRD is estimated to be 10.1 (p = 0.0007, 95% confidence interval CI 2.76-25.95), but is not significantly elevated among second-degree relatives. The RR for dying with non-ESRD CKD among first- and second-degree relatives of individuals dying with non-ESRD CKD was 3.89 (p = 0.0051, 95% CI 1.43-8.46) and 3.11 (p = 0.04, 95% CI 0.85-7.95), respectively. The Genealogical Index of Familiality statistic demonstrated that the individuals dying with ESRD are significantly more related than expected in this population (p = 0.013); significant excess relatedness was also observed for individuals dying with non-ESRD CKD (p = 0.006), suggesting a familial component for both, with evidence for common environmental and genetic effects., Conclusion: The results of this analysis of individuals dying with ESRD and non-ESRD CKD supports a significant and independent familial component to both conditions, suggesting a heritable factor playing a role., (Copyright 2006 S. Karger AG, Basel)

Published

2006

12. Identification and study of Utah pseudo-isolate populations-prospects for gene identification.

Author

Cannon-Albright LA, Farnham JM, Thomas A, and Camp NJ

Subjects

Databases as Topic statistics & numerical data, Female, Founder Effect, Humans, Male, Neoplasms genetics, Selection, Genetic, Utah, Genetics, Population, Pedigree

Abstract

Isolate populations of varied types have proven powerful for gene identification for rare Mendelian disorders, and continue to show such promise for more complex phenotypes. Existing isolate populations are limited in the phenotypes available for study, and new population isolates are unlikely to arise. We utilize genealogical data available for the state of Utah, dating back to its European founders, to retrospectively define and examine pseudo-isolate subpopulations. These pseudo-isolate populations are defined by selection of a set of "founders" from the genealogical data, and then limitation of "immigration" by censoring of matings and offspring that do not match the isolate population design. A wide variety of pseudo isolate and other study designs are possible by varying the number and type of founders and the extent of immigration allowed. We present several different example Birth-Country pseudo-isolate populations defined within the Utah Population Database (UPDB). We utilize linked cancer phenotype data available for the Utah population to show the utility of this pseudo-isolate approach for identification of more genetically homogeneous prostate cancer pedigrees for predisposition gene identification. In conclusion, we present a unique approach to retrospective "creation" of isolate populations using existing genealogical data. We use the UPDB to exhibit the utility of this approach for the highly heterogeneous Utah population, and suggest the approach is feasible for any population for which high quality genealogy and phenotype data are available., ((c) 2005 Wiley-Liss, Inc.)

Published

2005

13. Predisposition locus for major depression at chromosome 12q22-12q23.2.

Author

Abkevich V, Camp NJ, Hensel CH, Neff CD, Russell DL, Hughes DC, Plenk AM, Lowry MR, Richards RL, Carter C, Frech GC, Stone S, Rowe K, Chau CA, Cortado K, Hunt A, Luce K, O'Neil G, Poarch J, Potter J, Poulsen GH, Saxton H, Bernat-Sestak M, Thompson V, Gutin A, Skolnick MH, Shattuck D, and Cannon-Albright L

Subjects

Chromosome Mapping, Genetic Testing, Genome, Human, Humans, Microsatellite Repeats genetics, Pedigree, Utah, Chromosomes, Human, Pair 12 genetics, Depressive Disorder, Major genetics, Genetic Linkage genetics

Abstract

Major depression disorder is a common psychiatric disease with a major economic impact on society. In many cases, no effective treatment is available. The etiology of major depression is complex, but it is clear that the disease is, to a large extent, determined genetically, especially among individuals with a familial history of major depression, presumably through the involvement of multiple predisposition genes in addition to an environmental component. As a first step toward identification of chromosomal loci contributing to genetic predisposition to major depression, we have conducted a genomewide scan by using 628 microsatellite markers on 1,890 individuals from 110 Utah pedigrees with a strong family history of major depression. We identified significant linkage to major depression in males at marker D12S1300 (multipoint heterogeneity LOD score 4.6; P=.00003 after adjustment for multiple testing). With additional markers, the linkage evidence became highly significant, with the multipoint heterogeneity LOD score at marker D12S1706 increasing to 6.1 (P=.0000007 after adjustment for multiple testing). This study confirms the presence of one or more genes involved in psychiatric diseases on the q arm of chromosome 12 and provides strong evidence for the existence of a sex-specific predisposition gene to major depression at 12q22-q23.2.

Published

2003

14. A candidate prostate cancer susceptibility gene at chromosome 17p.

Author

Tavtigian SV, Simard J, Teng DH, Abtin V, Baumgard M, Beck A, Camp NJ, Carillo AR, Chen Y, Dayananth P, Desrochers M, Dumont M, Farnham JM, Frank D, Frye C, Ghaffari S, Gupte JS, Hu R, Iliev D, Janecki T, Kort EN, Laity KE, Leavitt A, Leblanc G, McArthur-Morrison J, Pederson A, Penn B, Peterson KT, Reid JE, Richards S, Schroeder M, Smith R, Snyder SC, Swedlund B, Swensen J, Thomas A, Tranchant M, Woodland AM, Labrie F, Skolnick MH, Neuhausen S, Rommens J, and Cannon-Albright LA

Subjects

Amino Acid Sequence, Cloning, Molecular methods, DNA, Complementary genetics, Founder Effect, Genetic Linkage, Genetic Predisposition to Disease, Genotype, Humans, Male, Molecular Sequence Data, Mutation, Missense, Pedigree, RNA, Messenger genetics, Sequence Analysis, DNA, Sequence Homology, Amino Acid, Utah, Chromosomes, Human, Pair 17 genetics, Neoplasm Proteins genetics, Prostatic Neoplasms genetics

Abstract

It is difficult to identify genes that predispose to prostate cancer due to late age at diagnosis, presence of phenocopies within high-risk pedigrees and genetic complexity. A genome-wide scan of large, high-risk pedigrees from Utah has provided evidence for linkage to a locus on chromosome 17p. We carried out positional cloning and mutation screening within the refined interval, identifying a gene, ELAC2, harboring mutations (including a frameshift and a nonconservative missense change) that segregate with prostate cancer in two pedigrees. In addition, two common missense variants in the gene are associated with the occurrence of prostate cancer. ELAC2 is a member of an uncharacterized gene family predicted to encode a metal-dependent hydrolase domain that is conserved among eukaryotes, archaebacteria and eubacteria. The gene product bears amino acid sequence similarity to two better understood protein families, namely the PSO2 (SNM1) DNA interstrand crosslink repair proteins and the 73-kD subunit of mRNA 3' end cleavage and polyadenylation specificity factor (CPSF73).

Published

2001

15. Prostate cancer susceptibility locus HPC1 in Utah high-risk pedigrees.

Author

Neuhausen SL, Farnham JM, Kort E, Tavtigian SV, Skolnick MH, and Cannon-Albright LA

Subjects

Aged, Disease Susceptibility, Genotype, Humans, Lod Score, Male, Microsatellite Repeats, Middle Aged, Pedigree, Penetrance, Risk Factors, Utah, Chromosomes, Human, Pair 1 genetics, Prostatic Neoplasms genetics

Abstract

A prostate cancer susceptibility locus ( HPC1 ) at 1q24-25 has been identified. Subsequent analysis showed that the majority of the evidence for localization was provided by families with relatively young (<65 years) average age at diagnosis. We examined evidence for linkage to this region in a set of 41 extended multi-case prostate cancer pedigrees containing 440 prostate cancer cases. Genotyping of five short tandem repeat markers in the region was performed on DNA from 1724 individuals, including 284 prostate cancer cases. In comparison with the families reported in the initial localization, the Utah pedigrees are generally much larger (average of 10.7 versus 5.1 cases) and have an older average age at diagnosis (69 versus 65 years). Two- and three-point linkage analyses were conducted using a previously reported model and provided replication for HPC1 (two-point: LOD = 1.73, P = 0.005 at D1S196; three-point: LOD = 2.06, P = 0.002 for the interval D1S196-D1S416 ). The youngest quartile (by median age at diagnosis) yielded a maximum LOD of 2.82, P = 0. 0003 (at D1S215-D1S222 ), compared with a maximum LOD of 0.73, P = 0. 07 for the oldest quartile pedigrees at the same locus. Further analysis with an age-dependent model, specifying higher sporadic rates for older cases, suggests that the linkage evidence may be lower than expected given the power of the resource due to a high sporadic rate in the large Utah pedigrees.

Published

1999

16. Familial associations between cancer sites.

Author

Thomas A, Cannon-Albright L, Bansal A, and Skolnick MH

Subjects

Cluster Analysis, Female, Genealogy and Heraldry, Genes, Tumor Suppressor, Humans, Male, Mutation, Neoplasms epidemiology, Utah epidemiology, Databases, Factual, Neoplasms genetics

Abstract

The Utah Population Database links together genealogical records, the Utah Cancer Registry, and Utah death certificates and allows identification of cancer clusters. Groups of individuals with cancers of some types tend to fall into related clusters within the genealogy. We examine the apparent tendency of cases of two types of cancer to cluster together and distinguish real clusters from chance occurrences. Some established associations are found, whereas some are surprisingly absent. Some new associations are also suggested., (Copyright 1999 Academic Press.)

Published

1999

17. Familial prostate cancer studies in Utah.

Author

Neuhausen SL, Skolnick MH, and Cannon-Albright L

Subjects

Aged, Aged, 80 and over, Chromosome Mapping, Genetic Predisposition to Disease, Humans, Male, Mass Screening, Middle Aged, Oncogenes genetics, Pedigree, Prostatic Neoplasms epidemiology, Risk Factors, Utah epidemiology, Prostatic Neoplasms genetics

Published

1997

18. Systematic population-based assessment of cancer risk in first-degree relatives of cancer probands.

Author

Goldgar DE, Easton DF, Cannon-Albright LA, and Skolnick MH

Subjects

Aged, Female, Humans, Male, Middle Aged, Neoplasms epidemiology, Risk Factors, Utah epidemiology, Neoplasms genetics

Abstract

Background: Cancer has long been recognized to have a familial component. Elevated risks for cancers at the same site for relatives of cancer probands have been reported for both common cancers and a number of the rarer cancer sites. For a particular cancer site, however, the estimated risks to relatives have varied considerably depending on criteria for selection of probands, how cancers were determined in relatives, and overall study design. Not surprisingly, the estimated risks of other cancers in relatives of probands with cancer at a given site have been subject to even more variation., Purpose: The aim of this study was to use the Utah Population Database resource to systematically study familial clustering of 28 distinct cancer site definitions among first-degree relatives (parents, siblings, and off-spring) of cancer probands., Methods: We estimated familial relative risks from the Utah Population Database by identifying all cases of cancer in these first-degree relatives. These observed values were compared with those expected based on cohort-specific internal rates calculated from 399,786 relatives of all individuals in the Utah Population Database known to have died in Utah., Results: All sites showed an excess of cancers of the same site among relatives, with thyroid and colon cancers and lymphocytic leukemia showing the highest familial risks. When the analyses were restricted to cases with early ages at diagnosis, increased familial components for most cancer sites became evident. A significant difference in familial relative risk (FRR) between male (FRR = 4.04; 95% confidence interval [CI] = 3.13-5.07) and female (FRR = 2.24; 95% CI = 1.54-3.08) probands was found for colon cancer. Highly significant familial associations (one-sided; P < .001) were found among breast, colon, and prostate cancers and between breast and thyroid cancers. Statistically significant (one-sided, P < .01) associations were also found between tobacco-associated sites (lung, larynx, lip, and cervix)., Conclusions: This study represents a unique comprehensive population-based study of familial cancer. The familial associations reported here will be useful in generating hypotheses about specific genetic and environmental factors that can be tested in genetic linkage and case-control studies.

Published

1994

19. Localization of the 9p melanoma susceptibility locus (MLM) to a 2-cM region between D9S736 and D9S171.

Author

Cannon-Albright LA, Goldgar DE, Neuhausen S, Gruis NA, Anderson DE, Lewis CM, Jost M, Tran TD, Nyguen K, and Kamb A

Subjects

Adult, Aged, Aged, 80 and over, Australia epidemiology, Chromosome Mapping, Europe ethnology, Female, Genetic Predisposition to Disease, Haplotypes genetics, Humans, Lod Score, Male, Melanoma epidemiology, Middle Aged, Netherlands epidemiology, Pedigree, Texas epidemiology, Utah epidemiology, Chromosomes, Human, Pair 9, Melanoma genetics

Abstract

A familial melanoma susceptibility locus (MLM) was identified on the short arm of chromosome 9 in a set of Utah and Texas kindreds. Subsequent confirmation was reported for a set of 26 Australian kindreds, a set of 7 Dutch kindreds, and a set of 13 NIH melanoma kindreds. The original localization report placed the locus near the IFNA-D9S126 interval on chromosome 9p. We report further localization using D9S171 and a newly developed marker, D9S736, both of which lie in the IFNA-D9S126 interval. Analysis of this set of kindreds places the melanoma susceptibility locus in a 2-cM region that is proximal to D9S736 and distal to D9S171.

Published

1994

20. Familiality of cancer in Utah.

Author

Cannon-Albright LA, Thomas A, Goldgar DE, Gholami K, Rowe K, Jacobsen M, McWhorter WP, and Skolnick MH

Subjects

Age Factors, Female, Humans, Male, Neoplasms epidemiology, Sex Factors, Utah epidemiology, Family, Neoplasms genetics, Registries

Abstract

The Utah Population Database allows examination of the genetic relationships among the 35.7% of all cancer cases in the state that have genealogical records. Familial clustering of cancer is measured by the Genealogical Index of Familiality and is examined by site, and within site by age of onset, histology, and gender. Most cancer sites examined show excess familiality for all cases considered together. Subsets of individuals with certain characteristics showed unusually high levels of familial clustering, specifically lymphocytic leukemias and especially chronic lymphocytic leukemia, lobular breast cancer, early lip cancer, early melanoma, and female lung cancers of alveolar/adenoma histology. These may represent characteristics of the most penetrant forms of inherited susceptibilities, those which are enhanced by environmental factors, chance aggregations, rare inherited syndromes, or a combination of these factors.

Published

1994

21. Chromosome 17q linkage studies of 18 Utah breast cancer kindreds.

Author

Goldgar DE, Cannon-Albright LA, Oliphant A, Ward JH, Linker G, Swensen J, Tran TD, Fields P, Uharriet P, and Skolnick MH

Subjects

Adult, Family Health, Female, Genetic Linkage, Genetic Markers, Heterozygote, Humans, Lod Score, Male, Middle Aged, Models, Genetic, Neoplastic Syndromes, Hereditary genetics, Ovarian Neoplasms genetics, Pedigree, Polymorphism, Genetic, Recombination, Genetic, Utah, Breast Neoplasms genetics, Chromosome Mapping methods, Chromosomes, Human, Pair 17, Proto-Oncogenes

Abstract

In this paper we present linkage results from the analysis of 18 Utah breast cancer kindreds, for three 17q markers. Four kindreds had LOD scores greater than 1.0 for at least one of the marker loci. One of these kindreds has a LOD score of 6.07 with D17S579, and we believe it to be the most informative 17q family reported to date. Among the kindreds which appear unlinked to 17q were an early-onset breast cancer family, a large breast-ovarian family, and a kindred with mixed age at onset. Analysis of individual recombinants in the linked families localizes the BRCA1 gene between THRA1 and D17S579 (Mfd188). A comparison of the Cancer and Steroid Hormone Study (CASH) model and a model which assumes a rare dominant susceptibility locus with low penetrance and no phenocopies stresses the difficulties in assessing linkage if the assumptions of the CASH model in terms of age at onset of breast cancer are not appropriate for the BRCA1 locus. A hypothetical breast cancer pedigree is used to calculate gene carrier probabilities under the CASH model, thereby illustrating some of our concerns regarding the use of this model to detect and exclude 17q linkage in breast cancer families.

Published

1993

22. Assignment of a locus for familial melanoma, MLM, to chromosome 9p13-p22.

Author

Cannon-Albright LA, Goldgar DE, Meyer LJ, Lewis CM, Anderson DE, Fountain JW, Hegi ME, Wiseman RW, Petty EM, and Bale AE

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Base Sequence, Child, Chromosome Aberrations, Dysplastic Nevus Syndrome genetics, Female, Genes, Tumor Suppressor, Genetic Markers, Humans, Lod Score, Male, Middle Aged, Molecular Sequence Data, Pedigree, Texas, Utah, Chromosomes, Human, Pair 9, Melanoma genetics, Skin Neoplasms genetics

Abstract

Linkage analysis of ten Utah kindreds and one Texas kindred with multiple cases of cutaneous malignant melanoma (CMM) provided evidence that a locus for familial melanoma susceptibility is in the chromosomal region 9p13-p22. The genetic markers analyzed reside in a candidate region on chromosome 9p21, previously implicated by the presence of homozygous deletions in melanoma tumors and by the presence of a germline deletion in an individual with eight independent melanomas. Multipoint linkage analysis was performed between the familial melanoma susceptibility locus (MLM) and two short tandem repeat markers, D9S126 and the interferon-alpha (IFNA) gene, which reside in the region of somatic loss in melanoma tumors. An analysis incorporating a partially penetrant dominant melanoma susceptibility locus places MLM near IFNA and D9S126 with a maximum location score of 12.71. Therefore, the region frequently deleted in melanoma tumors on 9p21 presumably contains a locus that plays a critical role in predisposition to familial melanoma.

Published

1992

23. Number, size, and histopathology of nevi in Utah kindreds.

Author

Meyer LJ, Goldgar DE, Cannon-Albright LA, Piepkorn MW, Zone JJ, Risman MB, and Skolnick MH

Subjects

Dysplastic Nevus Syndrome pathology, Humans, Melanoma pathology, Nevus pathology, Phenotype, Skin Neoplasms pathology, Utah, Dysplastic Nevus Syndrome genetics, Melanoma genetics, Nevus genetics, Skin Neoplasms genetics

Published

1992

24. Inheritance of nevus number and size in melanoma and dysplastic nevus syndrome kindreds.

Author

Goldgar DE, Cannon-Albright LA, Meyer LJ, Piepkorn MW, Zone JJ, and Skolnick MH

Subjects

Adolescent, Adult, Age Factors, Child, Dysplastic Nevus Syndrome pathology, Family, Female, Genes, Dominant, Genes, Recessive, Humans, Male, Melanoma pathology, Middle Aged, Phenotype, Sex Characteristics, Skin Neoplasms pathology, Utah, Dysplastic Nevus Syndrome genetics, Melanoma genetics, Skin Neoplasms genetics

Abstract

Previous studies of the genetics of melanoma have focused on the dysplastic nevus syndrome (DNS). The variability in clinical and histopathological expression of affected individuals, however, has made definition and diagnosis of the syndrome difficult and subjective. Independent of the DNS, case-control studies have demonstrated the total number of nevi to be a significant risk factor for melanoma. In this article, we report results of genetic analyses of two quantitative nevus phenotypes that can be measured objectively in all subjects: the total number of nevi on an individual (TNN) and total nevus density (TND), a derived phenotype which incorporates both number and size of nevi. Ten kindreds ascertained for multiple cases of DNS-melanoma (multiplex ascertainment) and 16 kindreds and 19 solitary cases ascertained from a sequential list of melanoma cases without regard for family history (simplex ascertainment) were studied. Both phenotypes exhibited increased levels in relatives of probands compared with those in spouse controls. While neither TNN nor TND exhibited evidence for a major factor in the simplex pedigrees, a major factor was strongly indicated in the multiplex kindreds for TND. When both phenotypes were examined in more detail in the multiplex kindreds, the phenotype incorporating nevus size, TND, fit a mendelian pattern of inheritance better than the TNN. Significant residual familial correlations were found for both phenotypes. Parameter estimates from the best fitting genetic model indicated that a major gene may be responsible for 55% of the phenotypic variability of TND in the multiplex kindreds.

Published

1991

25. Characteristics of familial colon cancer in a large population data base.

Author

Cannon-Albright LA, Thomas TC, Bishop DT, Skolnick MH, and Burt RW

Subjects

Adult, Age Factors, Aged, Aged, 80 and over, Colonic Neoplasms pathology, Disease Susceptibility, Humans, Middle Aged, Pedigree, Rectal Neoplasms pathology, Registries, Utah, Colonic Neoplasms genetics, Information Systems, Rectal Neoplasms genetics

Abstract

Early age onset and proximal colonic location are two specific characteristics of colon cancer which have been used clinically to assess the risk that an individual case is of familial rather than sporadic origin. This practice derives from the observation that these characteristics are typical of the rare, nonpolyposis inherited colorectal cancer syndromes. This study examines these two characteristics in cases of common colon cancer to determine whether they actually distinguish individuals at increased risk for familial colorectal cancer. Familial clusters of colon cancer in the Utah Population Data Base were examined. Common colon cancers were found to cluster excessively in families; however, the measure of familial clustering for distal colonic cases was increased to the same degree as proximal colonic cases. Early age onset was likewise not a distinguishing factor of familial cases. These results suggest that factors other than those that predispose to the rare syndromes are important in determining familial risk for common colon cancers, and that the absence of these two clinical features should not suggest the absence of familial risk of colorectal cancer.

Published

1989

26. The dysplastic melanocytic nevus: a prevalent lesion that correlates poorly with clinical phenotype.

Author

Piepkorn M, Meyer LJ, Goldgar D, Seuchter SA, Cannon-Albright LA, Skolnick MH, and Zone JJ

Subjects

Adolescent, Adult, Age Factors, Aged, Aged, 80 and over, Biopsy, Child, Dysplastic Nevus Syndrome epidemiology, Female, Humans, Male, Melanoma epidemiology, Middle Aged, Phenotype, Sex Factors, Utah, White People, Dysplastic Nevus Syndrome pathology

Abstract

We estimated the prevalence of persons with histologic dysplasia in at least one of two nevi examined by biopsy to be 53% in Utah's caucasians. This apparently high prevalence indicates that such lesions may represent a normal variant of a melanocytic nevus, perhaps those in the process of active proliferation. Regardless of the apparent ubiquity of these lesions, examination of biopsy specimens led to a grading scheme of histologic dysplasia that may reflect chronologic stages in the neoplastic development of melanocytic nevi. Comparison of these histologic findings with the clinical examination yielded the unexpected result that dysplasia and lesion size are independent of each other. Lesions 3 mm in diameter or smaller were as likely to be dysplastic as those much larger. There was, however, a statistically significant relationship between histologic dysplasia of a nevus examined by biopsy and the person's total number of melanocytic lesions. This finding indicates that the pathology grading scheme may be useful. The high prevalence of dysplastic nevi dilutes the clinical significance of a dysplastic nevus as an isolated finding and thereby lessens the importance of pathologic findings in the diagnosis of dysplastic nervus syndrome.

Published

1989

27. Segregation and linkage analysis of nine Utah breast cancer pedigrees.

Author

Bishop DT, Cannon-Albright L, McLellan T, Gardner EJ, and Skolnick MH

Subjects

Female, Genetic Markers, Humans, Pedigree, Space-Time Clustering, Utah, Breast Neoplasms genetics, Genetic Linkage, Models, Genetic, Neoplastic Syndromes, Hereditary

Abstract

The analysis of nine Utah families that were ascertained for clusters of breast cancer cases is reported. Segregation analysis of an inherited susceptibility to breast cancer shows two distinct maximum likelihood solutions that have almost equal likelihood. One model indicates that most females had zero risk for breast cancer, but 10% of the female population had risks much greater than the Utah age-specific incidence rates. The other model indicates that most females have a risk defined by the Utah rates for breast cancer, but a rare dominant gene is segregating for increased susceptibility to breast cancer. Our analysis shows that linkage results under the two models are consistent in sign but not in magnitude. No evidence for linkage was found with the 14 marker loci examined. In addition to demonstrating distortion of linkage results from ignoring sporadic cases, this analysis shows the inherent difficulty of obtaining parameter estimates for segregation analysis when families are ascertained from a cluster of cases.

Published

1988