Infrequently studied congenital anomalies as clues to the diagnosis of maternal diabetes mellitus

Frías, Jaime L.; Frías, Juan P.; Frías, Patricio A.; Martı́nez-Frı́as, María Luisa

doi:10.1002/ajmg.a.32071

Cited by 51 publications

(44 citation statements)

References 52 publications

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“…We conclude that the fetal genome controls the embryonic dysmorphogenesis in diabetic pregnancy by instigating a threshold level for the teratological insult and that the maternal genome controls the teratogenic insult by (dys)regulating the maternal metabolism. diabetes in pregnancy; congenital abnormalities; teratology; animal experimentation; aldose reductase; glyceraldehyde-3-phosphate dehydrogenase; sonic hedgehog homolog; ret proto-oncogene; glial-derived neurotrophic factor; antioxidative enzymes THE INCIDENCE OF CARDIOVASCULAR, skeletal, urinary, gastrointestinal, and caudal dysgenesis-related defects is higher in offspring of women with preexisting diabetes compared with infants of nondiabetic women (4,18,27,38). Despite extensive research and optimized clinical care, diabetic embryopathy has remained etiologically enigmatic and difficult to prevent (40).…”

mentioning

confidence: 99%

Genetic and environmental influence on diabetic rat embryopathy

Ejdesjö

Wentzel

Eriksson

2011

American Journal of Physiology-Endocrinology and Metabolism

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Ejdesjö A, Wentzel P, Eriksson UJ. Genetic and environmental influence on diabetic rat embryopathy. Am J Physiol Endocrinol Metab 300: E454 -E467, 2011. First published November 30, 2010 doi:10.1152/ajpendo.00543.2010We assessed genetic and environmental influence on fetal outcome in diabetic rat pregnancy. Crossing normal (N) and manifestly diabetic (MD) Wistar Furth (W) and Sprague-Dawley (L) females with W or L males yielded four different fetal genotypes (WW, LL, WL, and LW) in N or MD rat pregnancies for studies. We also evaluated fetal outcome in litters with enhanced or diminished severity of maternal MD state, denoted MD ϩ WL and MD Ϫ LW. The MDWW litters had less malformations and resorptions (0 and 19%) than the MDLL litters (17 and 30%). The MDWL litters (0 and 8%) were less maldeveloped than the MDLW litters (9 and 22%), whereas the MD ϩ WL (3 and 23%) and MD Ϫ LW (1 and 17%) litters showed increased and decreased dysmorphogenesis (compared with MDWL and MDLW litters). The pregnant MDW rats had lower serum levels of glucose, fructosamine, and branched-chain amino acids than the pregnant MDL rats, whereas the pregnant MD ϩ W and MD Ϫ L rats had levels comparable with those of the MDL and MDW rats, respectively. The 8-iso-PGF2␣ levels of the malformed MDLW offspring were increased compared with the nonmalformed MDLW offspring. Diabetes decreased fetal heart Ret and increased Bmp-4 gene expression in the MDLW offspring and caused decreased GDNF and Shh expression in the malformed fetal mandible of the MDLW offspring. We conclude that the fetal genome controls the embryonic dysmorphogenesis in diabetic pregnancy by instigating a threshold level for the teratological insult and that the maternal genome controls the teratogenic insult by (dys)regulating the maternal metabolism. diabetes in pregnancy; congenital abnormalities; teratology; animal experimentation; aldose reductase; glyceraldehyde-3-phosphate dehydrogenase; sonic hedgehog homolog; ret proto-oncogene; glial-derived neurotrophic factor; antioxidative enzymes THE INCIDENCE OF CARDIOVASCULAR, skeletal, urinary, gastrointestinal, and caudal dysgenesis-related defects is higher in offspring of women with preexisting diabetes compared with infants of nondiabetic women (4,18,27,38). Despite extensive research and optimized clinical care, diabetic embryopathy has remained etiologically enigmatic and difficult to prevent (40). The diabetes-induced alterations in embryonic development are similar to changes caused by several other teratogens, suggesting that the mechanism of diabetic dysmorphogenesis is multifactorial.The maternal environment and the fetal-maternal genotypes have been implicated in the teratogenicity of diabetic pregnancy. Thus, in diabetic women, the metabolic control (Hb A 1c levels) during the proximal part of the first trimester (29) is a strong predictor of the risk for congenital malformation (28). In experimental work, maternal metabolic deregulation has been confirmed as an important teratogenic factor (14,17,25), and a teratog...

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confidence: 99%

Genetic and environmental influence on diabetic rat embryopathy

Ejdesjö

Wentzel

Eriksson

2011

American Journal of Physiology-Endocrinology and Metabolism

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“…Almost any organ can be involved in malformations associated with maternal diabetes, including the cardiac and outflow tract, central nervous system, and the craniofacial, gastrointestinal, musculoskeletal, and urogenital systems (Ewart-Toland et al, 2000;Moore et al, 2000;Loffredo et al, 2001;Spilson et al, 2001, Wang et al, 2002Wren et al, 2003;Nielsen et al, 2005, Frias et al, 2007Lisowski et al, 2010). The types of anomalies seen are similar in infants of women with either DM1 or DM2 (Towner et al, 1995;Schaefer-Graf et al, 2000;Farrell et al, 2002, Dunne et al, 2003Macintosh et al, 2006).…”

Section: Introductionmentioning

confidence: 96%

Preconception care for women with diabetes and prevention of major congenital malformations

Kitzmiller¹,

Wallerstein

Correa

et al. 2010

Birth Defects Research

317

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This article provides an overview of the rationale for diabetes preconception care interventions for women with diabetes and the efficacy in reducing the excess occurrence of major congenital malformations. The problems with broad use of individualized preconception care are considered. In addition, suggestions are made for the implementation of more comprehensive interventions in the community and usual diabetes care settings, to address the multiple ongoing challenges in the prevention of structural anomalies associated with preexisting diabetes. Based on the published evidence, successful preconception care can be considered to include: achievement of individualized target standardized glycosylated hemoglobin levels, adequate nutrition, and minimizing hypoglycemia before and after discontinuing effective contraception and during the transition to early prenatal care.

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“…Various studies have investigated the RF for specific phenotypic subtypes, comprising bilateral renal agenesis/hypogenesis (RF = 11.91) [Correa et al, 2008] and multicystic dysplastic kidneys (RF = 6.15) [Frías et al, 2007].…”

Section: Maternal Diabetes and Malformationsmentioning

confidence: 99%

Diabetic Embryopathy: A Developmental Perspective from Fertilization to Adulthood

Castori¹

2012

Mol Syndromol

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Maternal diabetes mellitus is one of the strongest human teratogens. Despite recent advances in the fields of clinical embryology, experimental teratology and preventive medicine, diabetes-related perturbations of the maternofetal unit maintain a considerable impact on the Healthcare System. Classic consequences of prenatal exposure to hyperglycemia encompass (early) spontaneous abortions, perinatal death and malformations. The spectrum of related malformations comprises some recurrent blastogenic monotopic patterns, i.e. holoprosencephaly, caudal dysgenesis and oculoauriculovertebral spectrum, as well as pleiotropic syndromes, i.e. femoral hypoplasia-unusual face syndrome. Despite this, most malformed fetuses display multiple blastogenic defects of the VACTERL type, whose (apparently) casual combination preclude recognizing recurrent patterns, but accurately testifies to their developmental stage at onset. With the application of developmental biology in modern medicine, the effects of diabetes on the unborn patient are expanded to include the predisposition to develop insulin resistance in adulthood. The mechanisms underlying the transgenerational correlation between maternal diabetes and proneness to adult disorders in the offspring remain unclear, and the epigenetic plasticity may represent the missing link. In this scenario, a development-driven summary of the multifaced consequences of maternal diabetes on fertility and child health may add a practical resource to the repertoire of available information on early stages of embryogenesis.

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Infrequently studied congenital anomalies as clues to the diagnosis of maternal diabetes mellitus

Cited by 51 publications

References 52 publications

Genetic and environmental influence on diabetic rat embryopathy

Genetic and environmental influence on diabetic rat embryopathy

Preconception care for women with diabetes and prevention of major congenital malformations

Diabetic Embryopathy: A Developmental Perspective from Fertilization to Adulthood

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