Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations

AIMS/HYPOTHESIS: Caused by biallelic mutations of the gene encoding the transcription factor RFX6, the rare Mitchell–Riley syndrome (MRS) comprises neonatal diabetes, pancreatic hypoplasia, gallbladder agenesis or hypoplasia, duodenal atresia, and severe chronic diarrhea. So far, sixteen cases have...

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Autores principales: Passone, Caroline de Gouveia Buff, Vermillac, Gaëlle, Staels, Willem, Besancon, Alix, Kariyawasam, Dulanjalee, Godot, Cécile, Lambe, Cécile, Talbotec, Cécile, Girard, Muriel, Chardot, Christophe, Berteloot, Laureline, Hachem, Taymme, Lapillonne, Alexandre, Poidvin, Amélie, Storey, Caroline, Neve, Mathieu, Stan, Cosmina, Dugelay, Emmanuelle, Fauret-Amsellem, Anne-Laure, Capri, Yline, Cavé, Hélène, Ybarra, Marina, Chandra, Vikash, Scharfmann, Raphaël, Bismuth, Elise, Polak, Michel, Carel, Jean Claude, Pigneur, Bénédicte, Beltrand, Jacques
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9257252/
https://www.ncbi.nlm.nih.gov/pubmed/35813646
http://dx.doi.org/10.3389/fendo.2022.802351
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author Passone, Caroline de Gouveia Buff
Vermillac, Gaëlle
Staels, Willem
Besancon, Alix
Kariyawasam, Dulanjalee
Godot, Cécile
Lambe, Cécile
Talbotec, Cécile
Girard, Muriel
Chardot, Christophe
Berteloot, Laureline
Hachem, Taymme
Lapillonne, Alexandre
Poidvin, Amélie
Storey, Caroline
Neve, Mathieu
Stan, Cosmina
Dugelay, Emmanuelle
Fauret-Amsellem, Anne-Laure
Capri, Yline
Cavé, Hélène
Ybarra, Marina
Chandra, Vikash
Scharfmann, Raphaël
Bismuth, Elise
Polak, Michel
Carel, Jean Claude
Pigneur, Bénédicte
Beltrand, Jacques
author_facet Passone, Caroline de Gouveia Buff
Vermillac, Gaëlle
Staels, Willem
Besancon, Alix
Kariyawasam, Dulanjalee
Godot, Cécile
Lambe, Cécile
Talbotec, Cécile
Girard, Muriel
Chardot, Christophe
Berteloot, Laureline
Hachem, Taymme
Lapillonne, Alexandre
Poidvin, Amélie
Storey, Caroline
Neve, Mathieu
Stan, Cosmina
Dugelay, Emmanuelle
Fauret-Amsellem, Anne-Laure
Capri, Yline
Cavé, Hélène
Ybarra, Marina
Chandra, Vikash
Scharfmann, Raphaël
Bismuth, Elise
Polak, Michel
Carel, Jean Claude
Pigneur, Bénédicte
Beltrand, Jacques
author_sort Passone, Caroline de Gouveia Buff
collection PubMed
description AIMS/HYPOTHESIS: Caused by biallelic mutations of the gene encoding the transcription factor RFX6, the rare Mitchell–Riley syndrome (MRS) comprises neonatal diabetes, pancreatic hypoplasia, gallbladder agenesis or hypoplasia, duodenal atresia, and severe chronic diarrhea. So far, sixteen cases have been reported, all with a poor prognosis. This study discusses the multidisciplinary intensive clinical management of 4 new cases of MRS that survived over the first 2 years of life. Moreover, it demonstrates how the mutations impair the RFX6 function. METHODS: Clinical records were analyzed and described in detail. The functional impact of two RFX6(R181W) and RFX6(V506G) variants was assessed by measuring their ability to transactivate insulin transcription and genes that encode the L-type calcium channels required for normal pancreatic beta-cell function. RESULTS: All four patients were small for gestational age (SGA) and prenatally diagnosed with duodenal atresia. They presented with neonatal diabetes early in life and were treated with intravenous insulin therapy before switching to subcutaneous insulin pump therapy. All patients faced recurrent hypoglycemic episodes, exacerbated when parenteral nutrition (PN) was disconnected. A sensor-augmented insulin pump therapy with a predictive low-glucose suspension system was installed with good results. One patient had a homozygous c.1517T>G (p.Val506Gly) mutation, two patients had a homozygous p.Arg181Trp mutation, and one patient presented with new compound heterozygosity. The RFX6(V506G) and RFX6(R181W) mutations failed to transactivate the expression of insulin and genes that encode L-type calcium channel subunits required for normal pancreatic beta-cell function. CONCLUSIONS/INTERPRETATION: Multidisciplinary and intensive disease management improved the clinical outcomes in four patients with MRS, including adjustment of parenteral/oral nutrition progression and advanced diabetes technologies. A better understanding of RFX6 function, in both intestine and pancreas cells, may break ground in new therapies, particularly regarding the use of drugs that modulate the enteroendocrine system.
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spelling pubmed-92572522022-07-07 Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations Passone, Caroline de Gouveia Buff Vermillac, Gaëlle Staels, Willem Besancon, Alix Kariyawasam, Dulanjalee Godot, Cécile Lambe, Cécile Talbotec, Cécile Girard, Muriel Chardot, Christophe Berteloot, Laureline Hachem, Taymme Lapillonne, Alexandre Poidvin, Amélie Storey, Caroline Neve, Mathieu Stan, Cosmina Dugelay, Emmanuelle Fauret-Amsellem, Anne-Laure Capri, Yline Cavé, Hélène Ybarra, Marina Chandra, Vikash Scharfmann, Raphaël Bismuth, Elise Polak, Michel Carel, Jean Claude Pigneur, Bénédicte Beltrand, Jacques Front Endocrinol (Lausanne) Endocrinology AIMS/HYPOTHESIS: Caused by biallelic mutations of the gene encoding the transcription factor RFX6, the rare Mitchell–Riley syndrome (MRS) comprises neonatal diabetes, pancreatic hypoplasia, gallbladder agenesis or hypoplasia, duodenal atresia, and severe chronic diarrhea. So far, sixteen cases have been reported, all with a poor prognosis. This study discusses the multidisciplinary intensive clinical management of 4 new cases of MRS that survived over the first 2 years of life. Moreover, it demonstrates how the mutations impair the RFX6 function. METHODS: Clinical records were analyzed and described in detail. The functional impact of two RFX6(R181W) and RFX6(V506G) variants was assessed by measuring their ability to transactivate insulin transcription and genes that encode the L-type calcium channels required for normal pancreatic beta-cell function. RESULTS: All four patients were small for gestational age (SGA) and prenatally diagnosed with duodenal atresia. They presented with neonatal diabetes early in life and were treated with intravenous insulin therapy before switching to subcutaneous insulin pump therapy. All patients faced recurrent hypoglycemic episodes, exacerbated when parenteral nutrition (PN) was disconnected. A sensor-augmented insulin pump therapy with a predictive low-glucose suspension system was installed with good results. One patient had a homozygous c.1517T>G (p.Val506Gly) mutation, two patients had a homozygous p.Arg181Trp mutation, and one patient presented with new compound heterozygosity. The RFX6(V506G) and RFX6(R181W) mutations failed to transactivate the expression of insulin and genes that encode L-type calcium channel subunits required for normal pancreatic beta-cell function. CONCLUSIONS/INTERPRETATION: Multidisciplinary and intensive disease management improved the clinical outcomes in four patients with MRS, including adjustment of parenteral/oral nutrition progression and advanced diabetes technologies. A better understanding of RFX6 function, in both intestine and pancreas cells, may break ground in new therapies, particularly regarding the use of drugs that modulate the enteroendocrine system. Frontiers Media S.A. 2022-06-22 /pmc/articles/PMC9257252/ /pubmed/35813646 http://dx.doi.org/10.3389/fendo.2022.802351 Text en Copyright © 2022 Passone, Vermillac, Staels, Besancon, Kariyawasam, Godot, Lambe, Talbotec, Girard, Chardot, Berteloot, Hachem, Lapillonne, Poidvin, Storey, Neve, Stan, Dugelay, Fauret-Amsellem, Capri, Cavé, Ybarra, Chandra, Scharfmann, Bismuth, Polak, Carel, Pigneur and Beltrand https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Passone, Caroline de Gouveia Buff
Vermillac, Gaëlle
Staels, Willem
Besancon, Alix
Kariyawasam, Dulanjalee
Godot, Cécile
Lambe, Cécile
Talbotec, Cécile
Girard, Muriel
Chardot, Christophe
Berteloot, Laureline
Hachem, Taymme
Lapillonne, Alexandre
Poidvin, Amélie
Storey, Caroline
Neve, Mathieu
Stan, Cosmina
Dugelay, Emmanuelle
Fauret-Amsellem, Anne-Laure
Capri, Yline
Cavé, Hélène
Ybarra, Marina
Chandra, Vikash
Scharfmann, Raphaël
Bismuth, Elise
Polak, Michel
Carel, Jean Claude
Pigneur, Bénédicte
Beltrand, Jacques
Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations
title Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations
title_full Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations
title_fullStr Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations
title_full_unstemmed Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations
title_short Mitchell–Riley Syndrome: Improving Clinical Outcomes and Searching for Functional Impact of RFX-6 Mutations
title_sort mitchell–riley syndrome: improving clinical outcomes and searching for functional impact of rfx-6 mutations
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9257252/
https://www.ncbi.nlm.nih.gov/pubmed/35813646
http://dx.doi.org/10.3389/fendo.2022.802351
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