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Transcript 
Di George syndrome
22q11.2 deletion syndrome
AGE <2
AGE 2-18
European J Ped Nov 2004
IMMUNOLOGIC FEATURES
Aplasia-Hypoplasia Thymus

Variable immunological defects
( from normal to severe combined immunodeficiency)
20-40% DGS + immunological defects are not
associated with conotruncal cardiac defects
IMMUNOLOGICAL CLASSIFICATION
Complete DGS
Partial DGS
-   CD3/CD4/CD8
-  CD3/CD4/CD8
- No T cell response
to mitogens
- /N proliferation
tests in vitro
-    CD45RA,TREC
-  CD45RA,TREC
-    TCRBV
-  TCRBV
DGS with normal T cell subset
PARTIAL DGS
- Frequent
-  T cells/ n/  proliferation test
- Humoral defects
- Autoimmunity
- variable therapy
Infections in
22q11.2 deletion syndrome
-No symptoms
- Recurrent respiratory infections
-Other infections (rare)
virus,mastoiditi, osteomielitis)
(recurrent parotitis , papilloma
HUMORAL DEFECTS
Hypo-Hypergammaglobulinemia IgG
 IgA ,  IgM
 Subtypes IgG
 anticorpi specific antibody response (antipneumococcal,
antitetanous, antihaemofilus)
Jawad 2001, Kornfeld 2000, Smith 1998, Jennery 2003, Chinen 2003
FACTORS INFLUENCING
INFECTIONS IN DGS
•Immunodeficit/Allergy
•Anatomical Anomalies
(ear, larinx, trachea, atresia coane)
•Reflux gastroaesophagus
•Congenital heart disease
•Malnutrition
ORL
DGS e Autoimmunity
Autoimmune manifestation (10%)
•
NO CORRELATION T cell values
but
•
 T CD4+CD25+
Sullivan KE, 2002
Play a role in development of
autoimmunity
AUTOIMMUNITY
• Autoantibody
• JCA
• Trombocytopenia (Bernard-Soulier)
• Hemolitic anemia
• Tiroiditis
• Raynaud
• Urticaria
• Vitiligo
• Psoriasis
• RA corea
• Cerebellitis?
Jawad 2001, Kornfeld 2000, Smith 1998, Jennery 2003 Chinen 2003
T CELLS IN DGSp
•T CELL VALUES ARE DECREASED COMPARED
WITH AGE MATCHED HEALTHY DONORS
BUT
• THEY
ARE
INFECTIONS
NOT
PREDICTIVE
Sullivan K 2001
OF
Kinetics of the T-cell receptor CD4 and CD8 V
repertoire and immune function in DGSp to
determine the extent and nature of the
immunodeficiency and to correlate it to clinical
and immunological findings
Humoral
compartment by analyzing antibody
response in vivo and by immunophenotyping B cell
subsets in peripheral blood
Patient.
Sex
F.U.
CHD
Facies
Hypocal
Thymus
FISH
Infections
Treatme nt
1
M
65mo
IAA,
AVSD
+
-
Hypoplasia
+
Antibiotic phrophylaxis
2
M
51mo
TA
+
+
Absent
+
Recurrent Pneumonia,
URI,
Candidosis,
Recurrent OM,URI
3
M
37mo
IAA, AVSD
+
+
Absent
+
Recurrent OM, URI
4
M
44mo
ASD,PS
+
+
Absent
+
None
5
M
33mo
ASD
+
+
Absent
+
Pneumonia, Recurrent
OM, URI,
Antibiotic phrophylaxis
6
F
14mo
VSD
+
+
Normal
+
None
None
7
M
24mo
+
+
Absent
+
URI
None
8
F
25mo
PA,
VSD
PA,
VSD
+
-
Hypoplasia
+
Antibiotic
phrophylaxis
9
M
6mo
+
-
Absent
+
10
M
78mo
IAA,
VSD
Absent
Septicaemia,
Recurrent Pneumonia,
URI,
None
+
-
Normal
+
URI
None
11
F
29mo
AVSD
+
-
Absent
+
None
None
12
M
29mo
VSD
+
+
Hypoplasia
+
None
None
13
M
41mo
TA
+
+
Hypoplasia
+
None
None
Antibiotic phrophylaxis
IVIG
Antibiotic phrophylaxis
IVIG
None
None
F.U. follow up;CHD, Congenital heart disease; Hypocal, hypocalcemia; F, female; M, male; Facies, dysmorphic facies; VS D, ventricular septal defect; AVSD,Atrioventricular
septal defect; IAA,interrupted aortic arch; PA, pulmonary atresia; PS, pulmonic stenosis;TA,truncus arteriosus;IVIG, intravenous immunoglobulin, OM, otitis media;URI, upper
respiratory tract infection.
Pt.
Age
CD3
(mm/3)
CD4
(mm/3)
CD45RA
/CD4
(mm/3)
CD45R0
/CD4
(mm/3)
CD8
(mm/3)
CD45RA
/ CD8
(mm/3)
CD16
(mm/3)
IgG
(Mg/dl)
IgA
(Mg/dl)
IgM
(Mg/dl)
IgG
subclass
(Mg/dl)
Isohem
Sp Ab
LTM
1(74)
643
392
165
227
141
70
70
486
423
1200
202
86
Low
1006
251
1250
5,9
33
Low
HIB
N
N
85
Low
IgG3
N
2(46)
992
702
665
327
315
227
3(68)
2151
1261
706
542
853
640
298
983
445
923
145
28
N
N
N
720
n.d.
n.d.
480
680
835
128
62
N
N
Low
HIB
N
4(57)
2440
1680
n.d.
n.d.
5(38)
787
427
217
210
202
317
85
1125
225
939
68
137
N
Low
N
2307
643
1624
893
893
1299
1461
437
26
58
n.d.
n.d.
Low
PCP;
Tet
N
6(12)
5115
2923
7(31)
1025
634
431
202
268
179
88
561
854
947
75
50
N
N
N
N
8(40)
1625
1161
697
464
387
271
116
541
310
859
147
254
n.d.
N
N
9(6)
1007
758
553
205
213
192
21
677
592
662
55
65
n.d.
n.d.
Low
PCP
n.d.
10(84)
909
476
333
143
298
229
68
387
141
1190
100
50
N
N
N
N
11(30)
818
471
306
165
298
238
60
1066
545
689
38
30
N
Low
N
12(30)
1811
1180
826
354
665
552
113
1083
435
1600
91
96
N
n.d.
Low
PCP
N
13(42)
1834
1167
n.d.
n.d.
375
n.d.
n.d.
792
1417
827
229
61
N
N
n.d.
N
CD45R0 CD19
/CD8
(mm3)
(mm/3)
N
Pt: Patients; Age: months; FU: follow up;,:based on aged- matched controls; N:normal; n.d.:not done; Sp Ab:specific antibody response;
Isohem: Isohaemaglutinin titre; LTM:lymphocyte proliferation to mitogens.
N
N
N
N
N
SPECTRATYPING
Amplification of TCRBV
family by detection of
different segment of
CDR3
TCRBV DISTRIBUTION IN pDGS
(CD4 SUBSET)
100
90
T0
T1
80
70
60
50
40
30
20
10
0
Pazienti
TCRBV DISTRIBUTION IN pDGS
(CD8 SUBSET)
100
90
80
70
60
T0
T1
50
40
30
20
10
0
ID
K
Pazienti
Kinetics of TCRBV 13.2 (p2)
T=0
6 months of age
T1
TCR repertoire
in 22q11.2 deletion syndrome
•  alterations of TCR repertoire in CD8 subset
in
22q11.2 deletion syndrome patients compared to agematched healthy controls (Sullivan 2004, Pierdominici 2003)
(p=0,022)
• Improvement TCR repertoire distribution during followup
•  alterations of TCR repertoire in CD8 subset in DGSp
with recurrent infections (trend p>0.08)
•  TREC values
• These preliminary data suggest that TCR repertoire
alteration reflect altered T cell development (CD8 >CD4)
Kinetics of the T-cell receptor CD4 and CD8 V
repertoire and immune function in DGSp to
determine the extent and nature of the
immunodeficiency and to correlate it to clinical
and immunological findings
Humoral
compartment by analyzing antibody
response in vivo and by immunophenotyping B cell
subsets in peripheral blood
B CD27+
B natural effector CD27+ B CD27+ IgM-IgD- able to switch
•Rapid activation
IgM+ IgD+
•Primary response
•Class switch
•Polisaccharide antigens
(pneumococcal)
•Higher antibody affinity
•somatic permutation
B CD27+ are decreased in CVID, HIV , SCID-transplanted
CD27+ B CELLS in 22q11.2 DS
30
250
225
25
175
CD27+ B cells
(% of total B cells)
20
150
15
125
100
10
75
50
5
(P<0.01)
0
(P<0.05)
25
0
CD27+B cells (absolute numbers/m l)
200
IgM + IgD+ CD27+ B cells (% of total B cells)
20
18
16
2
0
125
14
100
12
10
75
8
6
50
4
(P<0.05)
(P<0.05)
25
0
IgM + IgD+ CD27+ B cells (absolute number)
CD27+ IgM+IgD+ B CELLS in 22q11.2 DS
150
CD27+ B CELLS in 22q11.2 DS
 CD27+ IgM+ IgD+ in 22q11.2 DS compared to agematched controls (p<0.05)
Decreased values of CD27 IgM+IgD+ could increased the risk of
recurrent infections in these patients
A
COMPLETE
EVALUATION
OF
IMMUNE
FUNCTION
INCLUDING IgD+ IgM+ CD27+ SUBSET AND HUMORAL
COMPARTMENT SHOULD BE CONSIDERED
IMMUNOLOGICAL EVALUATIONS
•T CELL PHENOTYPE
•Proliferation Test in vitro
•spectratyping
•IgG, IgA, IgM (subtypes)
•Specific antibody response
•autoantibody
•B cell maturation?
T
B
CONCLUSION I
•Variability of immunological alterations and of their
clinical expression does not allow easily to make a
standard protocol of diagnosis and therapy in DGS
•Further study in a larger number of patients could
contribute to select which immunological parameters
influence
the development of infections and
autoimmune diseases
CONCLUSION II
Because of the wide clinical spectrum an
optimal care of these patients is best
provided by a multidisciplinary team of
experts in a
Long-term follow-up
Natural history of 22q11.2 DS
Andrea Finocchi
Patrizia Ciaffi
Claudia Capponi
Maria Luisa Romiti
Silvia Di Cesare
Rita Carsetti
Paolo Rossi
Paediatric Hospital Bambino Gesù
Tor Vergata University - Rome
AGE< 1 Year
2-6 years
6 -18 years
Cardiac defect
Cardiac defect
Cardiac defect
A-Hypoplasia thymus
Immunodeficiency
Recurrent infections
Recurrent infections
(> otitis)
Immunodeficiency
Recurrent infections
Autoimmunity
Immunodeficiency
hypocalcemia
hypoparatiroidism
hypoparatiroidism
Feeding difficulties
Feeding difficulties
Cleft palate
Speech language
impairment
Speech language
impairment
Developmental delay
Behavioural delay
Behavioural delay
Learning difficulties
Others malformations
Others malformations
Others malformations
/scoliosis
Dysmorphic features
Dysmorphic features
Dysmorphic features
VACCINATION
Regular schedule
it is recommended :
• anti-HIB
• antipneumococcal
Immunological evaluation before measle vaccination
FIRST YEAR OF LIFE
THERAPY
• Clinical course
•ATB
• Immunoglobulins iv
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