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Literature DB >> 21327046

Why are levels of maternal microchimerism higher in type 1 diabetes pancreas?

Berendine Vanzyl¹, Raquel Planas, Yi Ye, Alan Foulis, Ronald R de Krijger, Marta Vives-Pi, Kathleen M Gillespie.

Abstract

Maternal microchimerism (MMc) results from transfer of maternal cells to the fetus in pregnancy. These cells have been shown to persist into adulthood in healthy individuals and an increased frequency of MMc has been associated with autoimmune disease. Female (presumed maternal) islet beta cells have recently been identified at higher levels in pancreas from a child with T1D compared to three controls. There was, however, no evidence that these cells were the targets of autoimmune attack. The aim of this study was to analyze well-characterized T1D pancreases encompassing a spectrum in age at diagnosis, and duration of diabetes, for the presence of maternal microchimerism compared to control pancreases.Pancreas samples were available from six males with T1D and four male controls. Fluorescent-labeled probes were used to detect X and Y chromosomes. At least 1,000 cells, usually 4,000-8,000 cells underwent confocal imaging for each pancreas. The frequency of MMc was higher in T1D pancreases (range 0.31-0.80%, mean 0.58%) than in controls (0.24-0.50%, mean 0.38%) (p = 0.05). Intriguingly, clusters of 2-3 MMc were occasionally found in the pancreases, particularly T1D pancreases, suggesting replication of these cells. Concomitant FISH and immunofluorescence staining for insulin or CD45 was performed to phenotype cells of maternal origin. Insulin positive and insulin negative MMc were identified indicating that MMc contribute to the exocrine and endocrine compartments. No CD45 positive MMc were observed. These data confirm the presence of maternal cells in human pancreas and support previous observations that levels of MMc are higher in T1D pancreas compared to controls. MMc do not appear to be immune effector cells and those that stain positive for insulin within intact islets in T1D tissue appear healthy with no evidence that they are the focus of immune attack. This study adds support to the hypothesis that maternal stem cells have the capacity to cross the placental barrier and differentiate into both endocrine and exocrine cells but more detailed characterization of MMc in the pancreas is required.

Entities: Chemical

Year: 2010 PMID： 21327046 PMCID： PMC3023622 DOI： 10.4161/chim.1.2.13891

Source DB: PubMed Journal: Chimerism ISSN： 1938-1964

20 in total

1. Cellular composition of pancreas-associated lymphoid tissue during human fetal pancreatic development.

Authors: E Korpershoek; P J M Leenen; H A Drexhage; R R De Krijger
Journal: Histopathology Date: 2004-09 Impact factor: 5.087

2. Maternal microchimerism in peripheral blood in type 1 diabetes and pancreatic islet beta cell microchimerism.

Authors: J Lee Nelson; Kathleen M Gillespie; Nathalie C Lambert; Anne M Stevens; Laurence S Loubiere; Joe C Rutledge; Wendy M Leisenring; Timothy D Erickson; Zhen Yan; Meghan E Mullarkey; Nick D Boespflug; Polly J Bingley; Edwin A M Gale
Journal: Proc Natl Acad Sci U S A Date: 2007-01-23 Impact factor: 11.205

3. Chimerism in children with juvenile dermatomyositis.

Authors: A M Reed; Y J Picornell; A Harwood; D W Kredich
Journal: Lancet Date: 2000 Dec 23-30 Impact factor: 79.321

4. Lineage tracing evidence for in vitro dedifferentiation but rare proliferation of mouse pancreatic beta-cells.

Authors: Noa Weinberg; Limor Ouziel-Yahalom; Sarah Knoller; Shimon Efrat; Yuval Dor
Journal: Diabetes Date: 2007-02-15 Impact factor: 9.461

5. The histopathology of the pancreas in type 1 (insulin-dependent) diabetes mellitus: a 25-year review of deaths in patients under 20 years of age in the United Kingdom.

Authors: A K Foulis; C N Liddle; M A Farquharson; J A Richmond; R S Weir
Journal: Diabetologia Date: 1986-05 Impact factor: 10.122

6. Microchimeric fetal cells cluster at sites of tissue injury in lung decades after pregnancy.

Authors: Keelin O'Donoghue; Hanan A Sultan; Faisal A Al-Allaf; Jonathan R Anderson; Josephine Wyatt-Ashmead; Nicholas M Fisk
Journal: Reprod Biomed Online Date: 2008-03 Impact factor: 3.828

7. Chimeric maternal cells with tissue-specific antigen expression and morphology are common in infant tissues.

Authors: Anne M Stevens; Heidi M Hermes; Meghan M Kiefer; Joe C Rutledge; J Lee Nelson
Journal: Pediatr Dev Pathol Date: 2009 Sep-Oct

8. Gene expression profiles for the human pancreas and purified islets in type 1 diabetes: new findings at clinical onset and in long-standing diabetes.

Authors: R Planas; J Carrillo; A Sanchez; M C Ruiz de Villa; F Nuñez; J Verdaguer; R F L James; R Pujol-Borrell; M Vives-Pi
Journal: Clin Exp Immunol Date: 2009-11-11 Impact factor: 4.330

9. Islet regeneration during the reversal of autoimmune diabetes in NOD mice.

Authors: Shohta Kodama; Willem Kühtreiber; Satoshi Fujimura; Elizabeth A Dale; Denise L Faustman
Journal: Science Date: 2003-11-14 Impact factor: 47.728

10. Beta cells can be generated from endogenous progenitors in injured adult mouse pancreas.

Authors: Xiaobo Xu; Joke D'Hoker; Geert Stangé; Stefan Bonné; Nico De Leu; Xiangwei Xiao; Mark Van de Casteele; Georg Mellitzer; Zhidong Ling; Danny Pipeleers; Luc Bouwens; Raphael Scharfmann; Gerard Gradwohl; Harry Heimberg
Journal: Cell Date: 2008-01-25 Impact factor: 41.582

12 in total

10. Chimeric cells of maternal origin do not appear to be pathogenic in the juvenile idiopathic inflammatory myopathies or muscular dystrophy.

Authors: Carol M Artlett; Sihem Sassi-Gaha; Ronald C Ramos; Frederick W Miller; Lisa G Rider
Journal: Arthritis Res Ther Date: 2015-09-04 Impact factor: 5.156

Why are levels of maternal microchimerism higher in type 1 diabetes pancreas?

1. Cellular composition of pancreas-associated lymphoid tissue during human fetal pancreatic development.

2. Maternal microchimerism in peripheral blood in type 1 diabetes and pancreatic islet beta cell microchimerism.

3. Chimerism in children with juvenile dermatomyositis.

4. Lineage tracing evidence for in vitro dedifferentiation but rare proliferation of mouse pancreatic beta-cells.

5. The histopathology of the pancreas in type 1 (insulin-dependent) diabetes mellitus: a 25-year review of deaths in patients under 20 years of age in the United Kingdom.

6. Microchimeric fetal cells cluster at sites of tissue injury in lung decades after pregnancy.

7. Chimeric maternal cells with tissue-specific antigen expression and morphology are common in infant tissues.

8. Gene expression profiles for the human pancreas and purified islets in type 1 diabetes: new findings at clinical onset and in long-standing diabetes.

9. Islet regeneration during the reversal of autoimmune diabetes in NOD mice.

10. Beta cells can be generated from endogenous progenitors in injured adult mouse pancreas.

1. Can maternal microchimeric cells influence the fetal response toward self antigens?

2. Maternal microchimerism in patients with biliary atresia: Implications for allograft tolerance.

3. Meeting report of the First Symposium on Chimerism.

Review 4. The prenatal environment and type 1 diabetes.

Review 5. Maternal-fetal cellular trafficking: clinical implications and consequences.

Review 6. The otherness of self: microchimerism in health and disease.

Review 7. Inherited nongenetic influences on the gut microbiome and immune system.

8. Maternal microchimerism in muscle biopsies from children with juvenile dermatomyositis.

Review 9. Maternal microchimerism: friend or foe in type 1 diabetes?

10. Chimeric cells of maternal origin do not appear to be pathogenic in the juvenile idiopathic inflammatory myopathies or muscular dystrophy.