Your search keyword '"Basson, Craig T."' showing total 8 results

1. Licogliflozin versus placebo in women with polycystic ovary syndrome: A randomized, double‐blind, phase 2 trial.

Author

Tan, Susanne, Ignatenko, Stanislav, Wagner, Frank, Dokras, Anuja, Seufert, Jochen, Zwanziger, Denise, Dunschen, Karin, Zakaria, Marjorie, Huseinovic, Neda, Basson, Craig T., Mahling, Ping, Fuhrer, Dagmar, and Hinder, Markus

Subjects

POLYCYSTIC ovary syndrome, INDUCED ovulation, INSULIN resistance, PLACEBOS, HYPERINSULINISM, TESTOSTERONE

Abstract

Polycystic ovary syndrome (PCOS) is characterized by hyperandrogenism and insulin resistance. The dual sodium‐glucose co‐transporter 1/2 inhibitor (SGLT1/2i) licogliflozin (LIK066) ameliorates hyperinsulinism in patients with diabetes and obesity. This study examines the effect of licogliflozin on androgens in women with PCOS. In a multicentre, randomized, placebo‐controlled, double‐blind, 2‐week trial, patients with PCOS received licogliflozin 50 mg or placebo three times a day (TID). Changes in free testosterone (FT), other androgens and variables of insulin resistance were analysed. Concentration of FT did not change (TRLIK066:TRPCB [FT]: 0.88; 90% CI: 0.70‐1.11; P =.353). Licogliflozin reduced androstendione (A4) by 19% (TRLIK066:TRPCB [A4]: 0.81; 90% CI: 0.68‐0.99; P =.089) and dehydroepiandrosteron sulphate (DHEAS) by 24% (TRLIK066:TRPCB [DHEAS]: 0.76; 90% CI: 0.65‐0.89; P =.008). Hyperinsulinaemia was reduced by 70% by licogliflozin (highest insulin concentration [MAXI]; TRLIK066:TRPCB [MAXI]: 0·26; 90% CI:0.20‐0.34; P <.001 and area under the curve insulin [AUCI]; TRLIK066:TRPCB [AUCI]: 0.32; 90% CI: 0.25‐0.41; P <.001). Diarrhoea and nausea occurred as common adverse events. Dual inhibition of SGLT1/2 ameliorates hyperinsulinaemia and hyperandrogenaemia in women with PCOS. Licogliflozin may represent a promising novel treatment option for PCOS. [ABSTRACT FROM AUTHOR]

Published

2021

2. Structural and Functional Genetic Disorders of the Great Vessels and Outflow Tracts.

Author

BEE, KATHARINE J., WILKES, DAVID, DEVEREUX, RICHARD B., LERMAN, BRUCE B., DIETZ, HARRY C., and BASSON, CRAIG T.

Subjects

GENETIC disorders, MOLECULAR genetics, MORPHOGENESIS, CARDIOVASCULAR system, GENETIC research

Abstract

Development of the aorta and pulmonary artery is a complex process involving multiple molecular genetic pathways that modulate morphogenesis of the outflow tracts and the anastomosis of branch vessels. Recent genetic studies of the cardiovascular system demonstrate that congenital and adult onset progressive disorders of the great vessels such as aneurysms are components of generalized vascular, cardiac, and extracardiovascular syndromes. Current paradigms suggest that aortic disease is founded in patterning anomalies of the conotruncus that occur in utero. These aberrations can be consequences of genetic aberrations in transcriptional regulation of signal transduction both within and outside the developing great vessels. [ABSTRACT FROM AUTHOR]

Published

2006

3. Molecular Genetic Analysis of PRKAG2 in Sporadic Wolff-Parkinson-White Syndrome.

Author

VAUGHAN, CARL J., HOM, YOLANDA, OKIN, DANIEL A., McDERMOTT, DEBORAH A., LERMAN, BRUCE B., and BASSON, CRAIG T.

Subjects

WOLFF-Parkinson-White syndrome, MOLECULAR genetics, GENETICS

Abstract

PRKAG2 Gene in Sporadic WPW Syndrome. Introduction: Mutations in the PRKAG2 gene that encodes the gamma2 regulatory subunit of AMP-activated protein kinase have been shown to cause autosomal dominant Wolff-Parkinson-White (WPW) syndrome associated with hypertrophic cardiomyopathy. Prior studies focused on familial WPW syndrome associated with other heart disease such as hypertrophic cardiomyopathy. However, such disease accounts for only a small fraction of WPW cases, and the contribution of PRKAG2 mutations to sporadic isolated WPW syndrome is unknown. Methods and Results: Subjects presented for clinical electrophysiologic evaluation of suspected WPW syndrome. WPW syndrome was diagnosed by ECG findings and/or by clinically indicated electrophysiologic study prior to enrollment. Echocardiography excluded hypertrophic cardiomyopathy. Denaturing high-performance liquid chromatography and automated sequencing were used to search for PRKAG2 mutations. Twenty-six patients without a family history of WPW syndrome were studied. No subject had cardiac hypertrophy, and only one patient had associated congenital heart disease. Accessory pathways were detected at diverse locations within the heart. Two polymorphisms in PRKAG2 were detected. [inv6+36insA] occurred in intron 6 in 4 WPW patients and [inv10+10delT] in intron 10 in 1 WPW patient. Both occurred in normal unrelated chromosomes. No PRKAG2 mutations were detected. Conclusion: This study shows that, unlike familial WPW syndrome, constitutional mutation of PRKAG2 is not commonly associated with sporadic WPW syndrome. Although polymorphisms within the PRKAG2 introns were identified, there is no evidence that these polymorphisms predispose to accessory pathway formation because their frequency is similarly high in both WPW patients and normal individuals. Further studies are warranted to identify the molecular basis of common sporadic WPW syndrome.(J Cardiovasc Electrophysiol, Vol. 14, pp. 263-268, March 2003). [ABSTRACT FROM AUTHOR]

Published

2003

4. Identification and localization of TBX5 transcription factor during human cardiac morphogenesis.

Author

Hatcher, Cathy J., Goldstein, Marsha M., Mah, Caroline S., Delia, C. Susan, and Basson, Craig T.

Published

2000

5. A t(2;19)(p13;p13.2) in a giant invasive cardiac lipoma from a patient with multiple lipomatosis.

Author

Vaughan, Carl J., Weremowicz, Stanislawa, Goldstein, Marsha M., Casey, Mairead, Hart, Matt, Hahn, Rebecca T., Devereux, Richard B., Girardi, Leonard, Schoen, Frederick J., Fletcher, Jonathan A., Morton, Cynthia C., and Basson, Craig T.

Published

2000

6. Interactions of Vascular Cells with Transforming Growth Factors-βa.

Author

MADRI, JOSEPH A., KOCHER, OLIVIER, MERWIN, JUNE R., BELL, LEONARD, TUCKER, ADELINE, and BASSON, CRAIG T.

Published

1990

7. Update: PGD and Holt-Oram syndrome.

Author

McDermott DA, He J, Song YS, Kligman I, and Basson CT

Subjects

Abnormalities, Multiple genetics, Female, Fertilization in Vitro, Humans, Infant, Newborn, Male, Mutation, Pregnancy, Pregnancy Outcome, Syndrome, T-Box Domain Proteins genetics, Abnormalities, Multiple diagnosis, Hand Deformities, Congenital diagnosis, Heart Defects, Congenital diagnosis, Preimplantation Diagnosis

Published

2005

8. Preimplantation genetic diagnosis of human congenital heart malformation and Holt-Oram syndrome.

Author

He J, McDermott DA, Song Y, Gilbert F, Kligman I, and Basson CT

Subjects

Adult, Chromosome Aberrations, DNA Mutational Analysis, Female, Fertilization in Vitro, Heart Defects, Congenital embryology, Humans, Male, Oocytes physiology, Syndrome, Hand Deformities, Congenital diagnosis, Hand Deformities, Congenital genetics, Heart Defects, Congenital diagnosis, Heart Defects, Congenital genetics, Preimplantation Diagnosis, T-Box Domain Proteins genetics

Abstract

Holt-Oram syndrome (HOS) is a multiple malformation syndrome associated with congenital heart malformation (CHM) and caused by mutations in the TBX5 transcription factor. Effective prenatal genetic diagnosis of HOS is limited by factors that modify clinical manifestations and confound prediction of an individual's phenotype. Although preimplantation genetic diagnosis (PGD) has been applied to complex disorders with some cardiovascular manifestations, its utility in Mendelian CHM has not been previously demonstrated. We tested whether PGD and in vitro fertilization (IVF) technology, including oocyte donation, can identify fertilized eggs affected by HOS for potential embryo selection. Five donor oocytes were fertilized in vitro with sperm from a HOS patient heterozygous for a Glu69ter-TBX5 mutation and then underwent embryo biopsy and genotyping. One carried the Glu69ter-TBX5 mutation; all others had wildtype genotypes. Two wildtype blastocysts were transferred to the mother, and the resulting singleton pregnancy was successfully delivered. Mutational analysis of fetal amniocytes and postpartum umbilical cord blood confirmed PGD. Fetal ultrasonography as well as postpartum electrocardiography and echocardiography also validated accurate prediction of normal skeletal and cardiac phenotypes. We conclude that PGD is an effective reproductive strategy for HOS patients. As more genetic etiologies for CHM are identified, application of PGD as adjunctive therapy to IVF will be increasingly available to prevent transmission of such diseases from affected parents to their children. Clinical application of PGD must balance the benefits of avoiding disease transmission with the medical risks and financial burdens of IVF., (Copyright 2003 Wiley-Liss, Inc.)

Published

2004