Your search keyword '"Brody, Lawrence"' showing total 10 results

1. KAREN ROTHENBERG'S (NOT SO) SECRET ROLES AND CONTRIBUTIONS AT THE U.S. NATIONAL INSTITUTES OF HEALTH.

Author

BERKMAN, BENJAMIN E., BRODY, LAWRENCE C., COLLINS, FRANCIS S., and GREEN, ERIC D.

Subjects

*BIOETHICS, *MEDICAL care laws

Abstract

The article acknowledges health law scholar Karen Rothenberg for her roles and contributions in the U.S. National Institutes of Health. Topics discussed include their mission to enhance health and reduce illness and disability, Rothenberg's interactions with the National Human Genome Research Institute and the Clinical Center's Department of Bioethics, and the importance of her role as Director of the Law and Health Care Program at the University of Maryland Law School in Baltimore.

Published

2020

2. Inherited BRCA2 mutations in African Americans with breast and/or ovarian cancer: a study of familial and early onset cases.

Author

Kanaan, Yasmine, Kpenu, Elikem, Utley, Kim, Adams-Campbell, Lucile, Dunston, Georgia M., Brody, Lawrence C., and Broome, Carolyn

Subjects

BREAST cancer, CANCER patients, AFRICAN Americans, GENETIC polymorphisms, CANCER

Abstract

In order to identify the spectrum of BRCA2 mutations in African Americans, breast or ovarian cancer patients from 74 independent families at elevated risk of germline mutations were investigated. The entire coding regions and flanking introns of BRCA2 were screened for germline mutations by single-stranded conformation polymorphism, protein truncation test, or denaturing high performance liquid chromatography followed by DNA sequencing. Eight distinct protein-truncating mutations were detected in six female patients (average age of onset of breast cancer: 37.6 years) and two male patients, but not in 163 unrelated disease-free controls. Two (1993delAA, 8643delAT) of the eight pathogenic mutations observed in African Americans have not been previously described. The other six pathogenic mutations (1882delT, 1991delATAA, 2001delTTAT, 2816insA, 4075delGT, 4088delA) have been detected in Caucasians; only the 2816insA mutation has been reported previously in African Americans. There were no significant differences in the frequency of deleterious BRCA2 mutations in African Americans compared with Caucasians. Six rare variations, not previously reported, were identified in five breast cancer patients but not in 163 disease-free control subjects. Of 11 different polymorphisms identified in high-risk African-American breast cancer patients, four may be unique to African Americans. An intron 10 polymorphism observed in patients was not detected in 163 disease-free African-American control subjects; this difference is statistically significant. Since many different pathogenic mutations and variants of unknown significance are observed in African Americans, BRCA2 genetic testing in high-risk African-American families must include the entire coding and flanking non-coding regions of the gene. [ABSTRACT FROM AUTHOR]

Published

2003

3. TAMRA and Its Impact on GSTT Planning Opportunities.

Author

Brody, Lawrence and Reilly, Edward F.

Subjects

LIFE insurance trusts, INHERITANCE & transfer tax, LAW

Abstract

Discusses the revisions made to the clauses of the Generation Skipping Transfer Tax (GSTT) by the Technical and Miscellaneous Revenue Act (TAMRA) of 1988. Exemption of irrevocable insurance trust from transfer tax under GSTT prior to the revision; Changes in the definition of the term trust by TAMRA; Strategies available after TAMRA revisions for funding an irrevocable insurance trust.

Published

1990

4. Use of Irrevocable Life Insurance Trusts in Estate Planning.

Author

Swirnoff, Michael A. and Brody, Lawrence

Subjects

IRREVOCABLE trusts, LIFE insurance trusts, LIFE insurance, TAX exemption, INSURANCE, GIFT taxes, LIFE insurance policies, INSURANCE policies

Abstract

The article describes the irrevocable life insurance trust as one of the most important tools available for creating tax-exempt wealth. The authors analyze also the income, gift and estate tax consequences of irrevocable life insurance trusts. The article starts with a discussion on the advantages of using a trust as the beneficiary of a life insurance policy. The authors analyze also the income, gift and estate tax consequences of irrevocable life insurance trusts. They point out the unresolved areas of which planners and drafters of irrevocable life insurance trusts will need to be aware of. The authors conclude that the use of irrevocable life insurance trust can maximize the availability of the policy proceeds to the grantor-insured's family by avoiding including those proceeds in either the grantor-insured's or his or her spouse's estate for tax purposes.

Published

1981

5. Split-Dollar Redux.

Author

Alexander, Neil and Brody, Lawrence

Subjects

SPLIT dollar life insurance policies, LIFE insurance policies, ACCOUNTANTS, INTERNAL revenue law

Abstract

This article explores the effect of the revenue notices and proposed regulations issued by the U.S. Internal Revenue Service in June 2003 on clients with split-dollar insurance plans. Under notice 2002-8 timing is critical when the employee computes insurance protection values using section 61. The key date for certified public accountants to remember is January 28, 2002. Plans entered into before this date must use table 2001, which is part of revenue notice 2001-10, to determine the value of life insurance protection the employer provides under the plan. Plans also can use the more favorable insurance company one-year term rates to determine the value of life insurance protection. A plan entered into after January 28, 2002, can use the insurer's published premium rates until January 1, 2004. Thereafter, for an employee to use these rates, the insurer must make them known to all persons who apply for term coverage and must use those rates when selling such coverage. That means the subsequent rates will be higher than those companies now are quoting.

Published

2003

6. Future Health Applications of Genomics: Priorities for Communication, Behavioral, and Social Sciences Research

Author

McBride, Colleen M., Bowen, Deborah, Brody, Lawrence C., Condit, Celeste M., Croyle, Robert T., Gwinn, Marta, Khoury, Muin J., Koehly, Laura M., Korf, Bruce R., Marteau, Theresa M., McLeroy, Kenneth, Patrick, Kevin, and Valente, Thomas W.

Subjects

*GENOMICS, *BEHAVIORAL research, *COMMUNICATIONS research, *SOCIAL science research, *PUBLIC health, *TRANSLATIONAL research, *BIOINFORMATICS, *HEALTH behavior

Abstract

Abstract: Despite the quickening momentum of genomic discovery, the communication, behavioral, and social sciences research needed for translating this discovery into public health applications has lagged behind. The National Human Genome Research Institute held a 2-day workshop in October 2008 convening an interdisciplinary group of scientists to recommend forward-looking priorities for translational research. This research agenda would be designed to redress the top three risk factors (tobacco use, poor diet, and physical inactivity) that contribute to the four major chronic diseases (heart disease, type 2 diabetes, lung disease, and many cancers) and account for half of all deaths worldwide. Three priority research areas were identified: (1) improving the public''s genetic literacy in order to enhance consumer skills; (2) gauging whether genomic information improves risk communication and adoption of healthier behaviors more than current approaches; and (3) exploring whether genomic discovery in concert with emerging technologies can elucidate new behavioral intervention targets. Important crosscutting themes also were identified, including the need to: (1) anticipate directions of genomic discovery; (2) take an agnostic scientific perspective in framing research questions asking whether genomic discovery adds value to other health promotion efforts; and (3) consider multiple levels of influence and systems that contribute to important public health problems. The priorities and themes offer a framework for a variety of stakeholders, including those who develop priorities for research funding, interdisciplinary teams engaged in genomics research, and policymakers grappling with how to use the products born of genomics research to address public health challenges. [Copyright &y& Elsevier]

Published

2010

7. Exome sequencing identifies novel genes underlying primary congenital glaucoma in the National Birth Defects Prevention Study.

Author

Blue EE, Moore KJ, North KE, Desrosiers TA, Carmichael SL, White JJ, Chong JX, Bamshad MJ, Jenkins MM, Almli LM, Brody LC, Freedman SF, Reefhuis J, Romitti PA, Shaw GM, Werler M, Kay DM, Browne ML, Feldkamp ML, Finnell RH, Nembhard WN, Pangilinan F, and Olshan AF

Subjects

Humans, Female, Male, United States, Mutation genetics, Genetic Predisposition to Disease, Infant, Infant, Newborn, Glaucoma genetics, Glaucoma congenital, Cytochrome P-450 CYP1B1 genetics, Exome Sequencing methods, Exome genetics

Abstract

Background: Primary congenital glaucoma (PCG) affects approximately 1 in 10,000 live born infants in the United States (U.S.). PCG has a autosomal recessive inheritance pattern, and variable expressivity and reduced penetrance have been reported. Likely causal variants in the most commonly mutated gene, CYP1B1, are less prevalent in the U.S., suggesting that alternative genes may contribute to the condition. This study utilized exome sequencing to investigate the genetic architecture of PCG in the U.S. and to identify novel genes and variants., Methods: We studied 37 family trios where infants had PCG and were part of the National Birth Defects Prevention Study (births 1997-2011), a U.S. multicenter study of birth defects. Samples underwent exome sequencing and sequence reads were aligned to the human reference sample (NCBI build 37/hg19). Variant filtration was conducted under de novo and Mendelian inheritance models using GEMINI., Results: Among candidate variants, CYP1B1 was most represented (five trios, 13.5%). Twelve probands (32%) had potentially pathogenic variants in other genes not previously linked to PCG but important in eye development and/or to underlie Mendelian conditions with potential phenotypic overlap (e.g., CRYBB2, RXRA, GLI2)., Conclusion: Variation in the genes identified in this population-based study may help to further explain the genetics of PCG., (© 2024 Wiley Periodicals LLC.)

Published

2024

8. A scoping review of social and behavioral science research to translate genomic discoveries into population health impact.

Author

Allen CG, Peterson S, Khoury MJ, Brody LC, and McBride CM

Subjects

Communication, Cross-Sectional Studies, Genomics, Humans, United States, Behavioral Sciences, Population Health

Abstract

Since the completion of the Human Genome Project, progress toward translating genomic research discoveries to address population health issues has been limited. Several meetings of social and behavioral scientists have outlined priority research areas where advancement of translational research could increase population health benefits of genomic discoveries. In this review, we track the pace of progress, study size and design, and focus of genomics translational research from 2012 to 2018 and its concordance with five social and behavioral science recommended priorities. We conducted a review of the literature following the Preferred Reporting Items for Systematic Reviews and Meta-Analysis Guidelines for Scoping Reviews. Steps involved completing a search in five databases and a hand search of bibliographies of relevant literature. Our search (from 2012 to 2018) yielded 4,538 unique studies; 117 were included in the final analyses. Two coders extracted data including items from the PICOTS framework. Analysis included descriptive statistics to help identify trends in pace, study size and design, and translational priority area. Among the 117 studies included in our final sample, nearly half focused on genomics applications that have evidence to support translation or implementation into practice (Centers for Disease Control and Prevention Tier 1 applications). Common study designs were cross-sectional (40.2%) and qualitative (24.8%), with average sample sizes of 716 across all studies. Most often, studies addressed public understanding of genetics and genomics (33.3%), risk communication (29.1%), and intervention development and testing of interventions to promote behavior change (19.7%). The number of studies that address social and behavioral science priority areas is extremely limited and the pace of this research continues to lag behind basic science advances. Much of the research identified in this review is descriptive and related to public understanding, risk communication, and intervention development and testing of interventions to promote behavior change. The field has been slow to develop and evaluate public health-friendly interventions and test implementation approaches that could enable health benefits and equitable access to genomic discoveries. As the completion of the human genome approaches its 20th anniversary, full engagement of transdisciplinary efforts to address translation challenges will be required to close this gap., (© Society of Behavioral Medicine 2020. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2021

9. Strategic vision for improving human health at The Forefront of Genomics.

Author

Green ED, Gunter C, Biesecker LG, Di Francesco V, Easter CL, Feingold EA, Felsenfeld AL, Kaufman DJ, Ostrander EA, Pavan WJ, Phillippy AM, Wise AL, Dayal JG, Kish BJ, Mandich A, Wellington CR, Wetterstrand KA, Bates SA, Leja D, Vasquez S, Gahl WA, Graham BJ, Kastner DL, Liu P, Rodriguez LL, Solomon BD, Bonham VL, Brody LC, Hutter CM, and Manolio TA

Subjects

Biomedical Research economics, COVID-19 genetics, Genomics economics, Humans, National Human Genome Research Institute (U.S.) economics, Social Change, Translational Research, Biomedical economics, United States, Biomedical Research trends, Genome, Human genetics, Genomics trends, Public Health standards, Translational Research, Biomedical trends

Abstract

Starting with the launch of the Human Genome Project three decades ago, and continuing after its completion in 2003, genomics has progressively come to have a central and catalytic role in basic and translational research. In addition, studies increasingly demonstrate how genomic information can be effectively used in clinical care. In the future, the anticipated advances in technology development, biological insights, and clinical applications (among others) will lead to more widespread integration of genomics into almost all areas of biomedical research, the adoption of genomics into mainstream medical and public-health practices, and an increasing relevance of genomics for everyday life. On behalf of the research community, the National Human Genome Research Institute recently completed a multi-year process of strategic engagement to identify future research priorities and opportunities in human genomics, with an emphasis on health applications. Here we describe the highest-priority elements envisioned for the cutting-edge of human genomics going forward-that is, at 'The Forefront of Genomics'.

Published

2020

10. Screening student athletes for sickle cell trait--a social and clinical experiment.

Author

Bonham VL, Dover GJ, and Brody LC

Subjects

Heterozygote, Humans, Organizational Policy, Organizations, Sports, Students, United States, Athletes, Mandatory Testing, Sickle Cell Trait diagnosis, Universities organization & administration

Published

2010