Preexisting pancreatic acinar cells contribute to acinar cell, but not islet β cell, regeneration

Desai, Biva M.; Oliver‐Krasinski, Jennifer; León, Diva D. De; Farzad, Cyrus; Hong, Nankang; Leach, Steven D.; Stoffers, Doris A.

doi:10.1172/jci29988

Cited by 279 publications

(245 citation statements)

References 33 publications

(21 reference statements)

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“…In this case, transient dedifferentiation of acinar cells is followed by acinar regeneration with no contribution of acinar lineage to ductal and endocrine lineages. The same conclusion was obtained from studies using Ppx in combination with acinar-specific lineage tracing (Desai et al, 2007). In the latter setting, Elastase-CreER T2 -labeled acini were only capable of producing acinar cells, but not ductal and endocrine cells.…”

Section: Injury-induced Reprogrammingsupporting

confidence: 70%

“…After about E14.5, acinar cells are mainly generated by the duplication of existing acinar cells, and endocrine progenitor birth in the trunk domain ends by the beginning of postnatal life (Zhou et al, 2007;Solar et al, 2009). Acinar cells and endocrine cells go through a maturation process lasting into postnatal life, and there is significant postnatal expansion of endocrine cell numbers, likely linked to self-replication (Desai et al, 2007;Finegood et al, 1995;Teta et al, 2007).…”

Section: The Secondary Transition: Onset Of Islet Duct and Acinar DImentioning

confidence: 99%

“…Studies on postnatal b-cell growth and proliferation have been reviewed extensively elsewhere and will not be covered in this review (reviewed in Ackermann and Gannon, 2007;Bonner-Weir et al, 2010). In order to compensate for body growth, acinar differentiation, maturation, and proliferation also continue after birth before gradually decreasing until weaning (Desai et al, 2007;Salpeter et al, 2010).…”

mentioning

confidence: 99%

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Pancreas organogenesis: From bud to plexus to gland

Pan

Wright

2011

Developmental Dynamics

510

580

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Pancreas oganogenesis comprises a coordinated and highly complex interplay of signaling events and transcriptional networks that guide a step-wise process of organ development from early bud specification all the way to the final mature organ state. Extensive research on pancreas development over the last few years, largely driven by a translational potential for pancreatic diseases (diabetes, pancreatic cancer, and so on), is markedly advancing our knowledge of these processes. It is a tenable goal that we will one day have a clear, complete picture of the transcriptional and signaling codes that control the entire organogenetic process, allowing us to apply this knowledge in a therapeutic context, by generating replacement cells in vitro, or perhaps one day to the whole organ in vivo. This review summarizes findings in the past 5 years that we feel are amongst the most significant in contributing to the deeper understanding of pancreas development. Rather than try to cover all aspects comprehensively, we have chosen to highlight interesting new concepts, and to discuss provocatively some of the more controversial findings or proposals. At the end of the review, we include a perspective section on how the whole pancreas differentiation process might be able to be unwound in a regulated fashion, or redirected, and suggest linkages to the possible reprogramming of other pancreatic cell-types in vivo, and to the optimization of the forward-directed-differentiation of human embryonic stem cells (hESC), or induced pluripotential cells (iPSC), towards mature b-cells. Developmental Dynamics 240:530-565,

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Section: Injury-induced Reprogrammingsupporting

confidence: 70%

Section: The Secondary Transition: Onset Of Islet Duct and Acinar DImentioning

confidence: 99%

mentioning

confidence: 99%

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Pancreas organogenesis: From bud to plexus to gland

Pan

Wright

2011

Developmental Dynamics

510

580

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“…Currently, there is little evidence that any other cell type contributes to β cell neogenesis. Although some studies had suggested the potential role of Pdx1 in promoting β cell transdifferentiation from acinar tissue [83,[104][105][106], a recent elegant lineage tracing analysis suggests that such cells do not contribute to new β cells in models of regeneration in vivo [107].…”

Section: Role Of Pdx1 In Adaptive β Cell Hyperplasia and β Cell Regenmentioning

confidence: 99%

A feat of metabolic proportions: Pdx1 orchestrates islet development and function in the maintenance of glucose homeostasis

Babu

Deering

Mirmira

2007

Molecular Genetics and Metabolism

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Emerging evidence over the past decade indicates a central role for transcription factors in the embryonic development of pancreatic islets and the consequent maintenance of normal glucose homeostasis. Pancreatic and duodenal homeobox 1 (Pdx1) is the best studied and perhaps most important of these factors. Whereas deletion or inactivating mutations of the Pdx1 gene causes whole pancreas agenesis in both mice and humans, even haploinsufficiency of the gene or alterations in its expression in mature islet cells causes substantial impairments in glucose tolerance and the development of a late-onset form of diabetes known as maturity onset diabetes of the young. The study of Pdx1 has revealed crucial phenotypic interrelationships of the varied cell types within the pancreas, particularly as these impinge upon cellular differentiation in the embryo and neogenesis and regeneration in the adult. In this review, we describe the actions of Pdx1 in the developing and mature pancreas and attempt to unify these actions with its known roles in modulating transcriptional complex formation and chromatin structure at the molecular genetic level.

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“…Ces limites ont réorienté les investigations vers des stratégies de différenciation in situ, sans recours à l'isolement et à la culture cellulaires. Au-delà de la controverse sur les capacités des cellules acinaires à produire spontanément de nouvelles cellules β lors de pancréatecto-mies ou autres lésions pancréatiques [42], il est admis que ces cellules sont capables de régénérer le pancréas exocrine [43]. Elles sont considérées à ce titre comme des progéniteurs facultatifs.…”

Section: Cellules Acinairesunclassified

La thérapie cellulaire du diabète

Lysy

2016

Med Sci (Paris)

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> La poss ibilité de remplacer des cellules β déficientes par de nouvelles cellules insulinosécrétantes chez le patient diabétique est démontrée par le succès de la transplantation d'îlots pancréatiques. Le manque de donneurs cadavériques a stimulé la recherche de sources alternatives de cellules β dont le palmarès est dominé par les cellules souches pluripotentes humaines pouvant acquérir des caractéristiques quasiment identiques à celles des cellules β et rétablir l'équilibre glycémique de souris diabétiques. Néanmoins, elles comportent un risque carcinogénique actuellement inévitable. Le pancréas adulte héberge des compartiments cellulaires aux capacités de transdifférenciation établies pouvant être exploitées pharmacologiquement in situ ou via des phases d'expansion en culture. Cette revue s'intéresse aux nouveaux développements concernant la thérapie cellulaire du diabète. < vie permettent de prévenir 60 % des DT2, il n'y a, à ce jour, aucune straté-gie de prévention du DT1 et les traitements actuels ne permettent pas d'atteindre les objectifs thérapeutiques tels que révélés par le dosage de l'hémoglobine glyquée (ou glycatée) (HbA1 C ) 2 [1]. Le DT1 est donc la cible des stratégies développées pour le remplacement des cellules β qui ont vu le jour en 1966 à Minneapolis avec la première greffe de pancréas humain combinée à une greffe de rein [2]. Après plus de 47 000 greffes d'organe (pancréas associé au rein ou pancréas seul), la technique a été nettement raffinée. Elle permet actuellement une survie des greffons d'environ 85 % à 1 an post-chirurgie [3], ce qui en fait une option thérapeutique pour des patients diabétiques en insuffisance rénale [4]. Cette technique n'est malgré tout pas généralisable étant donnés les degrés de morbidité et de mortalité associés au geste chirurgical (75 % de survie à 10 ans), la nécessité d'une immunosuppression à vie, et le manque de donneurs d'organe. Ces difficultés ont stimulé la recherche pour une thérapie cellulaire du diabète fondée sur des sources cellulaires variées comme les îlots pancréatiques 3 , les cellules souches pluripotentes ou les cellules somatiques adultes du pancréas. Transplantation des îlots pancréatiquesLa transplantation des îlots de Langerhans du pancréas humain s'est développée dans les années 1970, comme une alternative moins invasive à la greffe de pancréas entier. Cette technique a bénéficié de la 2 L'hémoglobine glyquée est une forme d'hémoglobine ayant subi une glycation, c'est-à-dire une addition non enzymatique de sucre sur la protéine. C'est un marqueur de la glycémie. 3 Les îlots pancréatiques, ou îlots de Langerhans sont formés de cellules endocrines capables de synthéti-ser l'insuline, le glucagon, la somatostatine et le polypeptide pancréatique.

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Preexisting pancreatic acinar cells contribute to acinar cell, but not islet β cell, regeneration

Cited by 279 publications

References 33 publications

Pancreas organogenesis: From bud to plexus to gland

Pancreas organogenesis: From bud to plexus to gland

A feat of metabolic proportions: Pdx1 orchestrates islet development and function in the maintenance of glucose homeostasis

La thérapie cellulaire du diabète

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