Top

Diabetologia

Published in:

01-09-2003 | Article

Maternal diabetes in the rat impairs the formation of neural-crest derived cranial nerve ganglia in the offspring

Authors: Dr. J. Cederberg, J. J. Picard, U. J. Eriksson

Published in: Diabetologia | Issue 9/2003

Abstract

Aims/hypothesis

Maternal diabetes mellitus increases the risk for fetal malformations. Several of these malformations are found in organs and tissues derived from the neural crest. Previous studies have shown changes in fetal organs of neural crest origin in experimental diabetes and changes in migration of neural crest cells exposed to high glucose in vitro.

Methods

We used whole-mount neurofilament staining of embryos from normal and diabetic mothers to investigate the development of cranial nerve ganglia. Neural tube explants were cultured in 10 and 40 mmol/l glucose and cell death and caspase activity was measured with flow cytometry.

Results

The development of cranial ganglia V, VII, VIII, IX and X was impaired in day 10–11 embryos of diabetic rats. There was also a higher rate of cell death of neural crest derived cells cultured in 40 mmol/l glucose for 20 h (35% compared to 12% in 10 mmol/l). However, exposure of cells to 40 mmol/l glucose in culture did not increase the activation of the cell death effector proteins-caspases-measured as cellular binding of the activated caspase marker VAD-FMK. This suggests that the cell death is not caused by caspase-dependent apoptosis or that the caspases are activated at an earlier stage.

Conclusion/interpretation

The development of neural crest-derived structures is disturbed already at the organogenic period in embryos of diabetic rats and this deteriorated development could be due to high-glucose induced increase in cell death of neural crest derived cells.

Casson I, Clarke C, Howard C et al.(1997) Outcomes of pregnancy in insulin dependent diabetic women: results of a five year population cohort study. BMJ 315:275–278PubMed

Hawthorne G, Robson S, Ryall EA, Sen D, Roberts SH, Ward Platt MP (1997) Prospective population based survey of outcome of pregnancy in diabetic women: results of the Northern Diabetic Pregnancy Audit. BMJ 315:279–281PubMed

Suhonen L, Hiilesmaa V, Teramo K (2000) Glycaemic control during early pregnancy and fetal malformations in women with type I diabetes mellitus. Diabetologia 43:79–82

Towner D, Kjos SL, Leung B et al.(1995) Congenital malformations in pregnancies complicated by NIDDM. Diabetes Care 18:1446–1451PubMed

Brydon P, Smith T, Proffitt M, Gee H, Holder R, Dunne F (2000) Pregnancy outcome in women with type 2 diabetes mellitus needs to be addressed. Int J Clin Pract 54:418–419PubMed

Eriksson UJ, Borg LAH, Cederberg J et al.(2000) Pathogenesis of diabetes-induced congenital malformations. Ups J Med Sci 105:53–84PubMed

Mills JL, Baker L, Goldman AS (1979) Malformations in infants of diabetic mothers occur before the seventh gestational week. Implications for treatment. Diabetes 28:292–293

Eriksson RSM, Thunberg L, Eriksson UJ (1989) Effects of interrupted insulin treatment on fetal outcome of pregnant diabetic rats. Diabetes 38:764–772PubMed

Ferencz C, Rubin JD, McCarter RJ, Clark EB (1990) Maternal diabetes and cardiovacular malformations: predominance of double outlet right ventricle and truncus arteriosus. Teratology 41:319–326PubMed

10.

Novak RW, Robinson HB (1994) Coincident DiGeorge anomaly and renal agenesis and its relation to maternal diabetes. Am J Med Genet 50:311–312PubMed

11.

Simán CM, Gittenberger-de Groot AC, Wisse B, Eriksson UJ (2000) Neural crest related malformations in offspring of diabetic rats decrease with vitamin E treatment. Teratology 61:355–367CrossRefPubMed

12.

Suzuki N, Svensson K, Eriksson UJ (1996) High glucose concentration inhibits migration of rat cranial neural crest cells in vitro. Diabetologia 39:401–411CrossRefPubMed

13.

Yang X, Borg LA, Eriksson UJ (1995) Altered mitochondrial morphology of rat embryos in diabetic pregnancy. Anat Rec 241:255–267PubMed

14.

Yang X, Borg LAH, Eriksson UJ (1997) Altered metabolism and superoxide generation in neural tissue of rat embryos exposed to high glucose. Am J Physiol 272:E173–E180PubMed

15.

Van Maele-Fabry G, Gofflot F, Clotman F, Picard JJ (1995) Alterations of mouse embryonic branchial nerves and ganglia induced by ethanol. Neurotoxicol Teratol 17:497–506CrossRefPubMed

16.

Gofflot F, Maele-Fabry G van, Picard JJ (1996) Cranial nerves and ganglia are altered after in vitro treatment of mouse embryos with valproic acid (VPA) and 4-en-VPA. Brain Res Dev Brain Res 93:62–69.CrossRefPubMed

17.

D'Amico-Martel A, Noden DM (1983) Contributions of placodal and neural crest cells to avian cranial peripheral ganglia. Am J Anat 166:445–468PubMed

18.

Eriksson UJ (1988) Importance of genetic predisposition and maternal environment for the occurrence of congenital malformations in offspring of diabetic rats. Teratology 37:365–374PubMed

19.

Tucker GC, Delarue M, Zada S, Boucaut JC, Thiery JP (1988) Expression of the HNK-1/NC-1 epitope in early vertebrate neurogenesis. Cell Tissue Res 251:457–465PubMed

20.

Erickson CA, Loring JF, Lester SM (1989) Migratory pathways of HNK-1-immunoreactive neural crest cells in the rat embryo. Dev Biol 134:112–118PubMed

21.

Nishida A, Kobayashi T, Ariyuki F (1997) In vitro developmental toxicity of concanavalin A in rat embryos: analysis of neural crest cell migration using monoclonal antibody HNK-1. Teratog Carcinog Mutagen 17:103–114CrossRefPubMed

22.

Dodd J, Morton SB, Karagogeos D, Yamamoto M, Jessell TM (1988) Spatial regulation of axonal glycoprotein expression on subsets of embryonic spinal neurons. Neuron 1:105–116PubMed

23.

Leist M, Jaattela M (2001) Four deaths and a funeral: from caspases to alternative mechanisms. Nat Rev Mol Cell Biol 2:589–598

24.

Durrieu F, Belloc F, Lacoste L et al.(1998) Caspase activation is an early event in anthracycline-induced apoptosis and allows detection of apoptotic cells before they are ingested by phagocytes. Exp Cell Res 240:165–175CrossRefPubMed

25.

Phelan SA, Ito M, Loeken MR (1997) Neural tube defects in embryos of diabetic mice. Role of the Pax-3 gene and apoptosis. Diabetes 46:1189–1197PubMed

26.

Fine EL, Horal M, Chang TI, Fortin G, Loeken MR (1999) Evidence that elevated glucose causes altered gene expression, apoptosis, and neural tube defects in a mouse model of diabetic pregnancy. Diabetes 48:2454–2462PubMed

27.

Conway SJ, Henderson DJ, Copp AJ (1997) Pax3 is required for cardiac neural crest migration in the mouse: evidence from the splotch (Sp2H) mutant. Development 124:505–514.PubMed

28.

Eriksson UJ, Borg LAH (1991) Protection by free oxygen radical scavenging enzymes against glucose-induced embryonic malformations in vitro. Diabetologia 34:325–331PubMed

29.

Eriksson UJ, Borg LA (1993) Diabetes and embryonic malformations. Role of substrate-induced free-oxygen radical production for dysmorphogenesis in cultured rat embryos. Diabetes 42:411–419PubMed

30.

Viana M, Herrera E, Bonet B (1996) Teratogenic effects of diabetes mellitus in the rat. Prevention with vitamin E. Diabetologia 39:1041–1046

31.

Cederberg J, Galli J, Luthman H, Eriksson UJ (2000) Increased mRNA levels of Mn-SOD and catalase in embryos of diabetic rats from a malformation-resistant strain. Diabetes 49:101–107PubMed

32.

Davis WL, Crawford LA, Cooper OJ, Farmer GR, Thomas DL, Freeman BL (1990) Ethanol induces the generation of reactive free radicals by neural crest cells in vitro. J Craniofac Genet Dev Biol 10:277–93PubMed

33.

Yasuda Y, Okamoto M, Konishi H, Matsuo T, Kihara T, Tanimura T (1986) Developmental anomalies induced by all-trans retinoic acid in fetal mice: I. Macroscopic findings. Teratology 34:37–49PubMed

34.

Kotch LE, Sulik KK (1992) Experimental fetal alcohol syndrome: proposed pathogenic basis for a variety of associated facial and brain anomalies. Am J Med Genet 44:168–176PubMed

35.

Dunty WC Jr, Chen SY, Zucker RM, Dehart DB, Sulik KK (2001) Selective vulnerability of embryonic cell populations to ethanol-induced apoptosis: implications for alcohol-related birth defects and neurodevelopmental disorder. Alcohol Clin Exp Res 25:1523–1535PubMed

36.

Yasuda Y, Konishi H, Kihara T, Tanimura T (1987) Developmental anomalies induced by all-trans-retinoic acid in fetal mice: II. Induction of abnormal neuroepithelium. Teratology 35:355–366PubMed

37.

Yasuda Y, Itoh K, Mizuno N, Konishi H, Tanimura T (1989) Alterations in migrating cranial neural crest cells in embryos of mice fed retinoic acid. Anal Cell Pathol 2:23–40PubMed

38.

Chan BW, Chan KS, Koide T et al. (2002) Maternal diabetes increases the risk of caudal regression caused by retinoic acid. Diabetes 51:2811–2816PubMed

39.

Calciu C, Kubow S, Chan HM (2002) Interactive dysmorphogenic effects of toxaphene or toxaphene congeners and hyperglycemia on cultured whole rat embryos during organogenesis. Toxicology 175:153–165CrossRefPubMed

40.

Sadler TW, Hunter ES, Wynn RE, Phillips LS (1989) Evidence for multifactorial origin if diabetes-induced embryopathies. Diabetes 38:70–74PubMed

41.

Buchanan TA, Denno KM, Sipos GF, Sadler TW (1994) Diabetic teratogenesis. In vitro evidence for a multifactorial etiology with little contribution from glucose per se. Diabetes 43:656–660PubMed

42.

Styrud J, Thunberg L, Nybacka O, Eriksson UJ (1995) Correlations between maternal metabolism and deranged development in the offspring of normal and diabetic rats. Pediatr Res 37:343–353PubMed

Title: Maternal diabetes in the rat impairs the formation of neural-crest derived cranial nerve ganglia in the offspring
Authors: Dr. J. Cederberg
J. J. Picard
U. J. Eriksson
Publication date: 01-09-2003
Publisher: Springer-Verlag
Published in: Diabetologia / Issue 9/2003
Print ISSN: 0012-186X
Electronic ISSN: 1432-0428
DOI: https://doi.org/10.1007/s00125-003-1100-1

Live Webinar | 27-06-2024 | 18:00 (CEST)

Keynote webinar | Spotlight on medication adherence

Reserve your place

Live: Thursday 27th June 2024, 18:00-19:30 (CEST)

WHO estimates that half of all patients worldwide are non-adherent to their prescribed medication. The consequences of poor adherence can be catastrophic, on both the individual and population level.

Join our expert panel to discover why you need to understand the drivers of non-adherence in your patients, and how you can optimize medication adherence in your clinics to drastically improve patient outcomes.

Prof. Kevin Dolgin

Prof. Florian Limbourg

Prof. Anoop Chauhan

Developed by: Springer Medicine

Obesity Clinical Trial Summary

At a glance: The STEP trials

A round-up of the STEP phase 3 clinical trials evaluating semaglutide for weight loss in people with overweight or obesity.

Developed by: Springer Medicine

Keynote webinar | Spotlight on medication adherence

Springer Medicine

Abstract

Aims/hypothesis

Methods

Results

Conclusion/interpretation

Please log in to get access to this content

Other articles of this Issue 9/2003

Apoptotic death of photoreceptors in the streptozotocin-induced diabetic rat retina

Haeme-oxygenase 1 expression in rat pancreatic beta cells is stimulated by supraphysiological glucose concentrations and by cyclic AMP

PAI-1 polymorphisms modulate phenotypes associated with the metabolic syndrome in obese and diabetic Caucasian population

Genetic control of non obese diabetic mice susceptibility to high-dose streptozotocin-induced diabetes

Suppressive effects of a selective inducible nitric oxide synthase (iNOS) inhibitor on pancreatic beta-cell dysfunction

Prevalence of diabetes and impaired fasting glucose in the Chinese adult population: International Collaborative Study of Cardiovascular Disease in Asia (InterASIA)

Keynote webinar | Spotlight on medication adherence

Live: Thursday 27th June 2024, 18:00-19:30 (CEST)

At a glance: The STEP trials