Post on 17-Oct-2019
U N I V E R S I T Ä T S M E D I Z I N B E R L I N
Uwe TrefzerKlinik für Dermatologie, Venerologie und
Allergologie
KNOTIGES BASALIOM
TeleangiektasienWachsartige glatte
Oberfläche
Basalzell Naevus Syndrom (Gorlin
Syndrom)
LH Goldberg, et al. Arch Dermatol 2010
„Old School“ vs. Targeted Therapies
Basalzell Naevus Syndrom (Gorlin
Syndrom)
LH Goldberg, et al. Arch Dermatol 2010
oral therapy with GDC-0449
Veratrum californicum -
Kalifornischer Germer
Cyclopamin
Hunting the Hedgehog
Binns, W., et al. Congenital cyclopian-type malformation in lambs induced by maternal ingestion of a
range plant, Veratrum californicum. Am. J. Vet. Res. 1963Keeler, R.F. et al. Teratogenic compounds of Veratrum californicum. Comparison of cyclopian effects
of steroidal alkaloids from the plant and structurally related compounds from other sources.
Teratology 1968
Hunting the Hedgehog
• Normaler HH Signalweg als Bestandteil embryonaler
Entwicklung und Zellwachstum
• Aberranter HH Signalweg bei ca. 25 % aller Tumoren des
Menschen nachgewiesen
Weiss GD, von Hoff DD. Clinical pharm Therap 2010
HH Inhibitor Studienstatus
GDC-0449 Phase II
BMS-833923 Phase I
IPI-926 Phase I
LDE-225 (Novartis) Phase I
PF-04449912 Phase I
GDC-0449 in der Behandlung multifokaler
Basalzellkarzinome (Basalzell-Naevus-Syndrom)
Therapie mit Imiquimod 5% Creme
E. Stockfleth et al
E. Stockfleth et al
Topische Therapie von AK mit 3%
Diclofenac in 2.5% Hyaluronsäure
Melanoma: Overall Survival by Stage
Survival (years)
Stage I (n=9175)
Stage II (n=5739)
Stage III (n=1528)
Stage IV (n=1158)
0 1 2 3 7 8 9 10 11 12 13 14 15654
0.9
0.8
0.7
0.6
0.5
0.4
0.3
0.2
0.1
0.0
Pro
port
ion S
urv
ivin
g
1.0
Adjuvante IFN-Therapie: Metaanalyse
• 6067 Patienten aus 10/13 publizierten Studien
zu IFN versus unbehandelte Kontrollen
• > 3.000 Todesfälle (für OS-Analyse) und >
3.700 „Rezidive“ (für RFS-Analyse)
auswertbar
Wheatley et al, ASCO 2007 (Abstract 8526)
Adjuvante IFN-Therapie: Metaanalyse
• Ergebnisse: RFS (OR = 0.87; CI 0.81-0.93)
p = 0.00006
OS (OR = 0.9; CI 0.84-0.97)
p = 0.008
• RFS und OS-Überlebensunterschied nach 5
Jahren: 7% bzw. 3%
Wheatley et al, ASCO 2007 (Abstract 8526)
Schema Dosis Frequenz Dauer Indikation
Niedrigdosis-
schema
3 Mio. IU
sc.
Tag 1,3 u. 5
jeder
Woche
18–24
MonateStad II – III
Hochdosis-
schema:
Initiierung
20 Mio IU/
m2
iv. als Kurz-
infusion
Tag 1-5
jeder
Woche
4 Wochen
Erhaltung10 Mio
IU/m2 sc.
Tag 1,3, u.
5 jeder
Woche
11 Monate Stad III
Stad III
Relapse Free Survival
Survival Time [months]
0 20 40 60
Su
rviv
al
Pro
bab
ilit
y
0,0
0,2
0,4
0,6
0,8
1,0
Arm A
Arm B
IFNa2a - 18 versus 60 Months
A.Hauschild et al.
Overall Survival
Survival Time [months]
0 20 40 60
Su
rviv
al
Pro
bab
ilit
y
0,0
0,2
0,4
0,6
0,8
1,0
Arm A
Arm B
IFNa2a - 18 versus 60 Months
A.Hauschild et al.
KNN Classifier
• MAGE-A3 screening
• Predictive signature to MAGE-A3 ASCI
MAGE-3-Protein-Signatur
AS15
HR: 0.29 [95% CI: 0.12 - 0.71]
KNN ClassifierLouahed, ASCO 2008
• MAGE-A3 screening
• Predictive signature to MAGE-A3 ASCI
Klinische Resultate mit MAGE3-Protein
im Stadium IV
Median
GS-: 2.3 months [95% CI: 2.3 - 4.4]
GS+: 10.3 months [95% CI: 6.7 - 12.4]HR: 0.31 [95% CI: 0.13 - 0.76]
AS15
Phase III study – DERMA
ADjuvant immunothERapy with MAGE-A3 in
melanomA
Resected MAGE-A3 (+) Stage IIIB/C Melanoma
Melanoma with macroscopic LN involvement
Randomization
Placebo MAGE-A3 ASCI
13 administrations over 27 months
1300 patients – double-blind, randomized trial
Melanoma: Overall Survival by Stage
Survival (years)
Stage I (n=9175)
Stage II (n=5739)
Stage III (n=1528)
Stage IV (n=1158)
0 1 2 3 7 8 9 10 11 12 13 14 15654
0.9
0.8
0.7
0.6
0.5
0.4
0.3
0.2
0.1
0.0
Pro
port
ion S
urv
ivin
g
1.0
• Lectin
• Elesclomol
• Genasense
• Maxamine
• Thymosin alpha
• Sorafenib
• HDAC-Inhibitor
• Cancer Vax („Morton Vakzine“)
• Vakzine
Chemoth.Targeted
Therapy
Ipilimumab Clinical
Study
1st line +++
not approved
+
2nd line +++ +
3rd line ++ (+)
Metastatic Melanoma
Activity of single agents in melanoma
DTIC 5-15%
Nitrosoureas 10-18%
Cisplatin 14-29%
IL-2 16%
Interferon- 10-14%
Taxol 14%
Vincristine 12%
.
Ives N J et al. JCO 2007;25:5426-5434
OR:
CT vs
BCT
.
Ives N J et al. JCO 2007;25:5426-5434
OS:
CT vs
BCT
Blockade CTLA-4
ASCO 2010
Ipilimumab
Ipilimumab
+
gp100 gp100
12 mo OS rate % 46 44 25
24 mo OS rate % 24 22 14
OS median mo 10.1 10.0 6.4
DCR % 28.5 20.1 11
O´Day et al.
O´Day et al.
June 5, 2011 (10.1056/NEJMoa1104621
EORTC 18071 Ipilimumab
Melanoma
Stage III (TxN1-3M0)
(N = 950)
Lymph node dissection
Randomisation within 56 days (1:1)
Arm A:
Ipilimumab (N=475)
Induction: 4 inf.. over 12 weeks
Maintenance: 1 inf every 12 w. for 3 years
or distant mets
Arm B:
Placebo (N=475)
as Arm A
Changes in the sum of diameters from
baseline by disease stage
Individual patients treated with vemurafenib
60
40
20
0
-20
-40
-60
-80
-100
M1a
M1b
M1c
Disease stage
Pe
rce
nt
ch
an
ge
fro
m b
as
eli
ne
in d
iam
ete
r o
f ta
rge
t le
sio
n
*******
* 7 Confirmed CRs
June 5, 2011
Chemoth.Targeted
Therapy
Ipilimumab Clinical
Study
1st line +
++
+
2nd line ++ +
3rd line ++ (+) (+) (+)
Metastatic Melanoma
55
The Future of Targeted Therapy for
Melanoma
Modified from K Flaherty
XL281
RG7204
GSK 21184338