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Endocrinology | 1999

A Low Protein Diet Alters the Balance of Islet Cell Replication and Apoptosis in the Fetal and Neonatal Rat and Is Associated with a Reduced Pancreatic Expression of Insulin-Like Growth Factor-II

J Petrik; Brigitte Reusens; Edith Arany; Claude Remacle; C. Coelho; Jj. Hoet; Dj. Hill

A programmed turnover of pancreatic beta cells occurs in the neonatal rat involving a loss of beta cells by apoptosis, and their replacement by islet cell replication and neogenesis. The timing of apoptosis is associated with a loss of expression of a survival factor, insulin-like growth factor-II (IGF-II), in the pancreatic islets. Offspring from rats chronically fed a low protein isocalorific diet (LP) exhibit a reduced pancreatic beta cell mass at birth and a reduced insulin secretion in later life. This study therefore investigated the impact of LP on islet cell ontogeny in the late fetal and neonatal rat, and any associated changes in the presence of IGFs and their binding proteins (IGFBPs). Pregnant Wistar rats were fed either LP (8% protein) or normal (C) (20% protein) chow from shortly after conception until the offspring were 21 days postnatal (PN). Bromo-deoxyuridine (BrdU) was administered 1 h before rats were killed and pancreata removed from animals between 19.5 days fetal life and postnatal day 21. Offspring of rats given LP diet had reduced birthweight, pancreatic beta cell mass, and pancreas insulin content, with smaller islets compared with control fed animals, which persisted to weaning. Histological analysis showed that islets from pups given LP diet had a lower nuclear labeling index with BrdU in the beta cells, although, paradoxically, more beta cells showed immunoreactivity for proliferating cell nuclear antigen (PCNA). Because PCNA is present in G1 as well as S phase of the cell cycle, we quantified the number of beta cells immunopositive for cyclin D1, a marker of G1, and NEK2, an indicator of cells in G2 and mitosis, More beta cells in islets from LP-fed animals contained cyclin D1, but less contained NEK2 than did those in controls. This suggests that the beta cell cycle may have a prolonged G1 phase in LP-fed animals in vivo. Offspring of rats given C diet had a low rate of islet cell apoptosis detected by the TUNEL method in fetal and neonatal life (1-2%), with a transient increase to 8% at PN day 14. Offspring of rats receiving LP diet demonstrated a significantly greater level of islet cell apoptosis at every age, rising to 15% at PN 14. IGF-II mRNA was quantified in whole pancreas and was significantly reduced in LP-fed animals at ages up to PN day 10. IGF-II immunoreactivity within the islets of LP-fed rats was also less apparent, but no changes were seen in immunoreactive IGF-I or IGFBPs-2 to -5. These findings show that LP diet changes the balance of beta cell replication and apoptosis in fetal and neonatal neonatal life, which may involve an altered length of beta cell cycle, and contribute to the smaller islet size and impaired insulin release seen in later life. A reduced pancreatic expression of IGF-II may contribute to the lower beta cell proliferation rate and increased apoptosis seen in the fetus and neonate after feeding LP diet.


Hormone and Metabolic Research | 1984

Cell Proliferation in Pancreatic Islets of Rat Fetuses and Neonates from Normal and Diabetic Mothers. An In Vitro and In Vivo Study

B. Reusensbillen; Claude Remacle; J. Daniline; Jj. Hoet


The Journal of Physiology | 1993

Low-protein Diet During Gestation in Rats - its Relevance To Human Non-insulin-dependent Diabetes

S. Dahri; A. Snoeck; B. Reusensbillen; Claude Remacle; Jj. Hoet


Diabetologia : clinical and experimental diabetes and metabolism | 1999

Effect of amino acids on beta cells and endothelial cells proliferation and in vitro interaction between the two cell types

S Boujendar; Brigitte Reusens; Jj. Hoet; Claude Remacle


Diabetologia : clinical and experimental diabetes and metabolism | 1998

Balance of islet cell birth and death of fetal and neonatal rats is altered by a low protein diet through mechanisms which include cell cycle kinetics

Brigitte Reusens; Dj. Hill; J Petrik; Claude Remacle; Jj. Hoet


Diabetologia : clinical and experimental diabetes and metabolism | 1997

Alterations in islets' insulin secretion of fetus from pregnant rats fed an isocaloric low protein diet

H. Cherif; Brigitte Reusens; S. Dahri; Claude Remacle; Jj. Hoet


Diabetologia : clinical and experimental diabetes and metabolism | 1997

Organs' vascularisation in offspring of pregnant rats fed an isocaloric protein restricted diet

Brigitte Reusens; IglesiasBarreira; N BennisTaleb; Claude Remacle; Jj. Hoet


Diabetologia : clinical and experimental diabetes and metabolism | 1996

Pancreatic blood flow and insulin release in adult rat fed a low protein diet pre and post-natally

IglesiasBarreira; Marie-Thérèse Ahn; Brigitte Reusens; S. Dahri; Claude Remacle; Jj. Hoet


Diabetologia : clinical and experimental diabetes and metabolism | 1996

Taurine stimulates insulin release of islets from rat fetus of mothers fed a normal diet but not low protein one.

H. Cherif; Brigitte Reusens; S. Dahri; Claude Remacle; Jj. Hoet


Diabetologia : clinical and experimental diabetes and metabolism | 1995

Taurine in the Culture-medium Enhances the Sensitivity of Fetal-rat Islets To Secretagogues

H. Cherif; S. Dahri; Brigitte Reusens; Claude Remacle; Jj. Hoet

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Brigitte Reusens

Lawson Health Research Institute

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Claude Remacle

Université catholique de Louvain

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Claude Remacle

Université catholique de Louvain

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S. Dahri

Université catholique de Louvain

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B. Reusensbillen

Université catholique de Louvain

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H. Cherif

Université catholique de Louvain

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Dj. Hill

University of Western Ontario

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J Petrik

University of Western Ontario

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IglesiasBarreira

Université catholique de Louvain

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L. Declercq

Université catholique de Louvain

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