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2 research outputs found

Investigating the Role of Islet Cytoarchitecture in Its Oscillation Using a New β-Cell Cluster Model

Author: A Nadal
A Sherman
A Sherman
A Sherman
AK Foulis
AL Hodgkin
Aparna Nittala
B Hellman
C Allefeld
C Schafer
CJ Rhodes
CL Zimliki
D Mears
DR Matthews
E Andreu
E Gylfe
E Samols
Edmund Crampin
EK Matthews
F Allagnat
F Bertuzzi
FC Jonkers
G de Vries
G De Vries
G Paolisso
G Paolisso
G Sohl
GM Ward
HP Meissner
I Atwater
I Atwater
I Quesada
J Aguirre
J Jo
JD Veldhuis
JI Stagner
JV Rocheleau
JV Sanchez-Andres
K Wierschem
K Yarimizu
LC Falke
M Brissova
M Perez-Armendariz
M Rosenblum
M Valdeolmillos
M Zarkovic
M Zarkovic
MA Ravier
MG Pedersen
MG Pedersen
N Porksen
O Cabrera
O Schmitz
P Bergsten
P Rorsman
P Smolen
PA Smith
PE MacDonald
PE MacDonald
PJ Bingley
PR Bratusch-Marrain
R Bertram
R Bertram
R Bertram
R Lehmann
RM Santos
RN Nlend
RR MacGregor
S Le Gurun
S O'Rahilly
Soumitra Ghosh
T Inoguchi
T Linn
T Sato
TA Kinard
TR Chay
TR Chay
W Gepts
Xujing Wang
Publication venue: Public Library of Science
Publication date: 03/10/2007
Field of study

The oscillatory insulin release is fundamental to normal glycemic control. The basis of the oscillation is the intercellular coupling and bursting synchronization of β cells in each islet. The functional role of islet β cell mass organization with respect to its oscillatory bursting is not well understood. This is of special interest in view of the recent finding of islet cytoarchitectural differences between human and animal models. In this study we developed a new hexagonal closest packing (HCP) cell cluster model. The model captures more accurately the real islet cell organization than the simple cubic packing (SCP) cluster that is conventionally used. Using our new model we investigated the functional characteristics of β-cell clusters, including the fraction of cells able to burst fb, the synchronization index λ of the bursting β cells, the bursting period Tb, the plateau fraction pf, and the amplitude of intracellular calcium oscillation [Ca]. We determined their dependence on cluster architectural parameters including number of cells nβ, number of inter-β cell couplings of each β cell nc, and the coupling strength gc. We found that at low values of nβ, nc and gc, the oscillation regularity improves with their increasing values. This functional gain plateaus around their physiological values in real islets, at nβ∼100, nc∼6 and gc∼200 pS. In addition, normal β-cell clusters are robust against significant perturbation to their architecture, including the presence of non-β cells or dead β cells. In clusters with nβ>∼100, coordinated β-cell bursting can be maintained at up to 70% of β-cell loss, which is consistent with laboratory and clinical findings of islets. Our results suggest that the bursting characteristics of a β-cell cluster depend quantitatively on its architecture in a non-linear fashion. These findings are important to understand the islet bursting phenomenon and the regulation of insulin secretion, under both physiological and pathological conditions

Public Library of Science (PLOS)

Crossref

PubMed Central

Islet-cell-to-cell communication as basis for normal insulin secretion

Author: Allagnat F
Belluardo N
Bosco D
Bosco D
Bruzzone R
Calabrese A
Calabrese A
Caton D
Charollais A
Cohen-Salmon M
Gilon P
Giordano E
Guldenagel M
Haefliger JA
Harris AL
Henquin JC
Herve JC
Herve JC
Iacobas DA
Jonkers FC
Kahn SE
Konstantinova I
Krattinger N
Kulkarni RN
Le Gurun S
Mears D
Meda P
Meda P
Meda P
Michon L
Moreno AP
O?Rahilly S
Orci L
Philippe J
Porksen N
Quesada I
Rocheleau JV
Schumann DM
Serre-Beinier V
Soria B
Speier S
Stefan Y
Theis M
Urschel S
Yamagata K
Zimliki CL
Publication venue: 'Wiley'
Publication date
Field of study

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