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M Polak1, 2, K Busiah1, 2, H Cavé3, A Bonnefond4, A Simon2,
I Flechtner2, A Dechaume4, N Pouvreau3, B Gerard4,
R Scharfmann1, P Froguel4, M Vaxillaire4.
French Network for the Study of NDM
INSERM U8451, Endocrinologie gynécologie et diabétologie pédiatriques2,
Université Paris Descartes, AP-HP, Hôpital Necker Enfants Malades ;
Biochimie génétique3, AP-HP, Hôpital Robert Debré, Paris ;
CNRS 8090 Institut Pasteur4, Lille.
Neonatal Hyperglycemia and Diabetes Mellitus
Presentation, mechanisms and new genes
Neonatal diabetes Mellitus
Introduction
Rare conditions
~ 1 : 100000 à 250.000
Various etiologies
• Immense progress made in the last 5 years
• Although rare
• Model to understand some aspects of normal development or
function
• Some genetic anomalies present in these patients may explain cases
of diabetes occuring later even at adult age
Difficult to manage
• Experienced team
Neonatal diabetes Mellitus
Clinical Presentation
2 main groups have been identified : permanent and
transient
A precise description of the clinical presentation of these
rare diseases was obtained through a multicenter study
in France
This cohort was collected retrospectively over a 30 years
period
Metz et al, Polak J of Ped 2002
Neonatal diabetes Mellitus Study
Features at birth and at diagnosis
PNDM
n = 21
TNDM
n = 29
Gestational age
(weeks)
39.2 ± 1.6
38.2 ± 2.2
p = 0.15
Birth weight (g)
2 497 ± 690
1 987 ± 510
p < 0.006
Birth length (cm)
47.5 ± 2.4
44.3 ± 3.4
p < 0.006
Head
circumference (cm)
33 ± 1.9
31.5 ± 1.8
p < 0.02
Intra-uterine
growth retardation
n = 7/19
36 %
n = 20/27
74 %
p < 0.03
Birth defects in 2 patients
- 1 TNDM patient with macroglossia
- 1 PNDM patients with heart defect
P value
Neonatal diabetes Mellitus Study
Features at birth and at diagnosis
PNDM
n = 21
TNDM
n = 29
P value
Gestational age
(weeks)
39.2 ± 1.6
38.2 ± 2.2
p = 0.15
Median age (days)
at diagnosis
(range)
27 (1-127)
6 (1-81)
p < 0.01
Initial insulin dose
(unit/kg/day)
1.4 ± 1.2
0.6 ± 0.25
p < 0.006
Neonatal Diabetes
Transient cases: chromosome 6
anomalies, promotor insulin gene,
Potassium channel
Permanent cases: insulin gene coding
sequences, Potassium channel
• Pancreatic Agenesis
• Glucokinase gene mutation
• IPEX
• Wolcott - Rallison Syndrome
• GLIS 3 (with hypothyroidism)
K+(ATP) channels in glucose metabolism
Link glucose metabolism – insulin secretion
Glucose
Glucose
Blood Glucose
Increase
INSULIN
SECRETION
Insulin
Glucose
Glucose
LOW
METABOLISM
Ca2+
Ca2+
ATP
Ca2+
MgADP
ATP
K+
MgADP
- 70 mV
Dépolarization
Hyperpolarization
K+
Closed K+(ATP) channel
Low glucose
High glucose
Normal Subject
Introduction: Kir6.2, potassium channel and
beta cell insulin secretion
NEJM 2004; 350:1817
A Gloyn et al., in A Hattersley laboratory reported in an ethnically diverse patient
cohort that heterozygous activating mutations in the KCNJ11 gene encoding
the Kir6.2 subunit of the pancreatic beta-cell potassium ATP (KATP) channel
cause PNDM and that some of these mutations are also associated
with developmental delay, muscle weakness and epilepsy
N Engl J Med 2004; 350:20
Kir6.2, the beta cell and permanent neonatal diabetesmellitus:
KCNJ11 mutations exist in about 50% of PNDM
NEJM 2004; 350:1817
The effect of drugs which increase insulin secretion
Were studied in these patients
Effects of sulfonylureas on beta cell
Ewan R Pearson*, Isabelle Flechtner*, Pal Njolstad* et al. NEJM 2006; 355: 467-477
Continuous glucose monitoring: child M.
Insulin pump
Glibenclamide
HbA1c
HbA1c under insulin 8,5%
(7,65-8,55)
HbA1c under sulfonylureas 6,4%
(6,19-6,61)
decrease of 1,7%
(12 weeks, p<0,001)
Identical levels at 1 year (n=12)
6% at 15 months (n=4)
5,7% at 2 years (n=1)
No increase in hypoglycemia
(CGMS®)
Physiopathology
Mutations in the ABCC8 gene/ SUR1in nine families
Andrey P. Babenko*, Michel Polak* ; N Engl J Med 2006; 355:456-66
PND12 (L213R)
NN
NN
PND16 (I1424V)
TND16 (L582V)
I
NA
NN
NN
2
1
1
2
NA
4
3
5
II
NM
NM
TND13 (C435R)
NA
TND19 (R1379C)
NN
NM
NM
1
NN
2
III
NM
NN
NN
6
NN
NM
TND28 (H1023Y)
NM
NN
6
NM
NM
I
TND17 (R1379C)
TND34 (R1182Q)
II
NA
NN
NN
NM
16
2
1
NM
NA
NN
3
NM
NM
4
G
III
NM
NN
TND36 (L582V)
1
2
3
4
5
6
7
IV
NN
NN
NA
NA
NM
NA
NA
NM
1
NN
V
NM
NM
Treatment with sulfonylureas
4 probands transferred from Insulin oral sulfonylureas
Proband
Mutation
Dominant
/de novo
Age at exam
[remission]
(year)
Insulin
(U/kg/day)
At transfer
Sulfonylurea
PND12
L213R
de novo
4.75
0.12
Glibenclamide
10 mg/j
I1424V
de novo
16.5
0.88
Glibenclamide
15 mg/j
R1379C
de novo
15.7
[6]
1.2
Glibenclamide
15 mg/j
H1023Y
de novo
16
[16]
0.5
Glipizide
10 mg/j
O
PND16
O
TND19
O
+
TND28
O
Father of TND 13 (C435R) was also transferred successfully
After 24 years of insulin injections
Dominant SUR1 mutations account for a significant fraction (~ 15%) of neonatal
diabetes cases, effectively treatable with oral hypoglycemic agents
Hôpital Necker
M. Polak
K Busiah
Biochimie
A Simon
génétique, Hôpital
JJ. Robert
Robert Debré,
I. Flechtner
Paris
P. Czernichow
H. Cave,
Equipe soignante
N Pouvreau,
B Gerard
S. Pereira,
C. Liger
Hormonologie
D Chevenne
CNRS 8090
Institut Pasteur,
Lille
M. Vaxillaire
P. Froguel
A. Bonnefond
A. Dechaume
U845 INSERM
R. Scharfmann
ENDOCRINOLOGUES DIABETOLOGUES
PEDIATRES
France
Pascal BARAT
Sylvie NIVOT ADAMIAK
Sabine BARON
Ramona NICOLESCU
Anne-Marie BERTRAND
Priscille PELISSIER
Elise BISMUTH
Myriam PEPIN-DONAT
Élisabeth BONNEMAISON
Sylvie PRADINES
Hélène BONY-TRIFUNOVIC Emmanuelle RAMOSMarie-Noëlle BORTOLUZZI
CALDAGUES
Henri BRUEL
Rachel REYNAUD
Jean Claude CAREL
Virginie RIBAULT
Régis COUTANT
Odile RICHARD
Hélène CROSNIER
Nicole SER
Fabienne DALLA-VALE
Gilbert SIMONIN
Christine DELCROIX
Sylvie SOSKIN
François DESPERT
Anne SPITERI
Marc DE KERDANET
Chantal STUCKENS
Brigitte DOREMUS
Véronique SULMONT
Clémentine DUPUIS
Lyse TAILLEBOIS
Patrick GARANDEAU
Nadia TUBIANA-RUFI
Iva GUEORGUIEVA
Valérie VENTURA
Caroline HASSELMANN
Jacques WEILL
Nourredine IDRES
Dominique KAUFFMANN
François KURTZ
Claire LE TALLEC
Anne LIENHARDT-ROUSSIE
Guy André LOEUILLE
Marie MANCINI
Chantal METZ
Brigitte MIGNOT
Denis MORIN
Les patients
Leurs familles
ANR, Erare, CIFRE
ENDOCRINOLOGUES
DIABETOLOGUES PEDIATRES
Monde
S. ABOURAZZAK
C. ACEIRINI
M. BEREGZASZI
V. BEAULOYE
C. CASTRO CORREIA
V. CRET
P. CROCK
T. DANNE
L. DE VRIES
M. DE VROEDE
N. DINI
U. EINBERG
L. FILIPPI
M. GONTHIER
M. HOWIDI
F. JENNANE
P.E. HAEREID
T. KAPPELEN
E. KHALLOUF
O. KORDONOURI
JL LECHUGA
M. MAES
P. MATON
I. MICLE
M. MIHU
R. NIMRI
G. PIERQUIN
M. PHILLIP
S. RIINA
S. SAINI
S. SARICI
V. SKRABIC
G. SZINNAI
D. TAHA
M. TURKMEN
N. VON DER WEID