Farmacogenetica bij targeted therapies

Farmacogenetica bij targeted therapies

Henk-Jan Guchelaar Klinische Farmacie & Toxicologie Amersfoort – 8 april 2010

Farmacogenetica

Mahgoub, A., R. & Smith, R. L. Lancet 1977(2): 584–586 Polymorphic hydroxylation of debrisoquine in man

CYP2D6 fenotype

debrisoquine/4-OH-debrisoquine

CYP2D6 genotype Allel

Enzym activiteit

Genetische variant

Allel frequentie (%) Caucasisch (Europa)

Japan

Tanzania

*1

Normaal

Wild-type

32.2-36.4

43

27.8

*2

Normaal

2850C>T, 4180G>C

28.5-32.4

12.3

40

*2x2

Hoog

Duplicatie

1-1.3

*3

Absent

2549delA

1-2

*4

Absent

1846G>A

17.2-20.7

.2

.9

*5

Absent

CYP2D6 deletie

2-6.9

4.5

6.3

*6

Absent

1707delT

.9-1.3

*9

Laag

2615_2617delAAG

1.8-2.7

*10

Laag

100C>T

1.5-2

*17

Laag

1023C>T, 2850C>T

*41

Laag

2988G>A

Fenotype:

0

0

38.1

3.8 17

8.4

Poor Metabolizer (5-10%) Intermediate Metabolizer (10-15%)

http://www.cypalleles.ki.se/

CYP2D6/2C19 varianten en chip technologie

• 33 CYP2D6 varianten • 3 CYP2C19 varianten

Van genotype naar phenotype

E

Roche, AmpliChip CYP450 Test, manual

Concept: concentratie-effect relatie Distributie, metabolisme, eliminatie absorptie

Concentratie-effect relatie

6 studies: 639 pt PD en 443 pt PK (sunitinib + SU12662) 2 studies “any solid tumor”; 2 studies GIST; 2 studies mRCC 25-150 mg/dag of om de dag in een 4/2, 2/2 en 2/1 week-schema Houk, Cancer Chemother Pharmacol, Dec 2009

Concentratie-effect relatie • Blootstelling (AUC)

~ TTP en OS ~ response ~ incidentie vermoeidheid

• Plasmaconcentratie

~ DBP

• Cum. Blootstelling

~ absolute aantal neutrofielen

mediane AUCss (> 0.8 ug*hr/mL) Houk, Cancer Chemother Pharmacol, Dec 2009

Concentratie-effect relatie

10

Houk, Cancer Chemother Pharmacol, Dec 2009

Orale cytostatica: transporters

Oostendorp, Cancer Treat Rev 2009;35(2):137-147

Resorptie: grote interpatient variabiliteit Mecano-studie: nierttransplantatie

Everolimus blood concentration (µg/L)

40

35

30

25

≈ 5-voud 20

15

10

5

0 -1

0

1

2

3

4

5

6

7

Time (Hours)

Unpublished data D.J. Moes

Variabiliteit in DNA • Farmacokinetiek geneesmiddelen • Transporters • Metabolisme

3% 3% 4% 12%

CYP1A2 CYP2E1 CYP2C19 CYP2C9

53% 25%

CYP2D6 CYP3A4

13

“drug targets” RCC

Rini , Lancet Oncology 2009 (modified)

Monogenetische eigenschap versus “complex” fenotype

Nebert, Drug Metab Rev 2008:187-224

15

Respons mRCC Drug

Patients

PFS

(number)

(months

RECIST SD response

median)

(%)

Withdrawal due adverse events

Previous

MSKCC

ECOG

Therapy

score >0

score 0

Disease sites ≥ 3

(%)

(%)

(%)

(%)

(%) sunitinib

375

11

48

8

no

62

62

57

sorafinib

97

5.7

74.5 (≥ 6 weeks)

11.3

no

44

57.7

-

pazopanib

225

12

44.9

15

yes- 31 cy

43

65

-

axitinib

62

7.4

17.7

35.5

yes-100 so

-

33.9

-

lapatinib

209

3.8 TTP

32

13

yes-100 cy

59

-

-

gefitinib

21

2.7

38.1

0

yes-100 cy

52.4

57

42.9

erlotinib

45

-

31

-

no

-

-

-

everolimus

41

11.2

57

-

63.4

-

34

temsirolimus

209

5.5

32.1

14

no

100

-

-

bevacizumab

50

11

58

20

no

100

-

38

(≥ 8 weeks)

yes- 83 cy

50% erlotinib

Farmacogenetica studies Drug

Disease

Gene

sunitinib

imatinib

danusertib

telatinib

Toxicity / response

Pharmacokinetic paramater

Study data will be presented

GIST

ABCB1

↓ oral clearance; no association CL

GIST

ABCG2

no association CL; ↓ clearance HT

Various solid tumors

ABCB1;

Various solid tumors

ABCB1;

no association neutropenia

no association CL

no association transporters with any toxicity grade 1-4

no association with exposure AUC

ABCG2

ABCG2

no association toxicity with VEGFR2 and VEGFR3 gefitinib

erlotinib

NSCLC

ABCB1

no association skin toxicity and diarrhoea

NSCLC

ABCG2

↑ diarrhoea HT

Various solid tumors

ABCG2;

HNSCC

ABCB1

HNSCC;

ABCG2

no association with diarrhoea

VEGFR2;

VEGR associates with OS and

VEGF

less grade 3 and 4 hypertension

no association with exposure

ABCB1 no association CL no association AUC; ↓ clearance HT

NSCLC bevacizumab

breastcancer

Pander, Curr Opin Mol Ther 2010 (submitted)

Metabolisme en transporters TKIs

Enzymen fase I

Sunitinib

CYP3A4

Sorafenib

CYP3A4

Axitinib

Pazopanib

Enzymen fase II

Transporters

ABCB1, ABCG2 UGT1A9

ABCB1, ABCG2

Major CYP3A4 Minor CYP1A2

unknown

Major CYP3A4 Minor CYP1A2, CYP2C8

ABCB1, ABCG2 Van Erp, Cancer Treat Rev 2009;35(8):692-706 Hurwitz, Clin Cancer Res 2009;15(12):4220-4227 Rugo, J Clin Oncol 2005;23(24):5474 – 5483 FDA registration information

Farmacogenetica sunitinib toxiciteit • Identificeren genetische markers die voorspellen voor sunitinib toxiciteit • 219 patienten behandeld met sunitinib (UMCG, VUMC, ErasmusMC, NKI, LUMC)

• mRCC (159), GIST (50), overig (10) • Toxiciteit geevalueerd in eerste cyclus (6 wk) NCI–CTC-AE versie 3.0 • Univariate associatie; gevolgd door multivariate logistische regressie analyse; correctie voor leeftijd, geslacht, ECOG; p- value < 0.05 • 31 ‘single nucleotide polymorphisms’ in 12 kandidaat genen – PK en PD sunitinib

19

Van Erp, J Clin Oncol 2009:27(26):4406-12

Selectie PK gerelateerde SNPs ABCG2 (BCRP) (421C/A, 34G/A, -15622C/T, 1143C/T) ABCB1 (Pgp) (3435C/T, 1236C/T, 2677G/T)

NR1I2 (-25385C/T, -24113G/A, 7635A/G, 8055C/T, 10620C/T, 10799G/A ) NR1I3 (5719C/T, 7738A/C, 7837T/G)

CYP3A4 (

Metabolieten

Sunitinib CYP3A5 (6986A/G)

SU12662 (actief) en inactieve metabolieten

CYP1A1 (2455A/G) CYP1A2 (-163A/C) O

N N H

N H O

F N H

20

Van Erp, J Clin Oncol 2009:27(26):4406-12

Selectie PD gerelateerde SNPs RET

1580T/C

738T/C

2251G/A

-604T/C

-1171C/G

-92G/A

-735G/A

54T/C

-573G/T

1191C/T

1501A/G 1501A/G

1718T/A

Van Erp, J Clin Oncol 2009:27(26):4406-12

21

‘Any toxicity’

% with any toxicity > grade 2 ABCG2 haplotype

% with any toxicity > grade 2 VEGFR genotype OR=2.39 P=0.046

OR=0.38 P=0.016 50 45 40 35 30 25 20 15 10 5 0

31,1 22,2 14,3

population

at least 1 copy of TT

no copy of TT

100 90 80 70 60 50 40 30 20 10 0

66,7

30,3

22,2

19

population

CC

CT

TT

Van Erp, J Clin Oncol 2009:27(26):4406-12

Leukopenie

% with leucopenia at 4 weeks OR= 6.24 P= 0.029

100

OR=1.74 P=0.041

100

86,7

80 60

59,5

54,9

40 20 0 population

AA

AG

GG

Cyp1A1 genotype

Van Erp, J Clin Oncol 2009:27(26):4406-12

Leukopenie % with leucopenia at 4 weeks OR= 0.36 P= 0.008

100 80 60

71 59,5 51,5

52,3

CT

CC

40 20 0

population

TT

FLT3 genotype 24

Van Erp, J Clin Oncol 2009:27(26):4406-12

Hand-foot syndroom en mucositis % hand-foot syndrome ABCB1 haplotype

% mucosal inflammation CYP1A1 genotype

OR=0.39 P=0.035

30 25 20 15 10 5 0

OR=4.03 P=0.021 86,7

100

25,5

80

19

60

10,5

44

40

40,7

20

0

0

population at least 1 copy no copy of of TTT TTT

population

AA

AG

GG

Van Erp, J Clin Oncol 2009:27(26):4406-12

Associaties toxiciteit met SNPs • Leukopenie • CYP1A1 2455A/G

OR= 6.24

• FLT3 738T/C

OR= 2.8

• NR1I3 haplotype

OR= 1.74

• Any toxicity > graad 2 • VEGFR2 1191C/T

OR= 2.39

• ABCG2 haplotype

OR= 2.63

• Mucositis • CYP1A1 2455A/G

OR= 4.03

• Handfoot syndroom • ABCB1 haplotype

OR= 2.56

26

Van Erp, J Clin Oncol 2009:27(26):4406-12

Leukopenie

27

Farmacogenetica sunitinib effectiviteit • Identificeren genetische markers die voorspellen voor sunitinib effectiviteit • PFS/OS • 136 mRCC ‘clear cell’

• 31 ‘single nucleotide polymorphisms’ in 12 kandidaat genen – PK en PD sunitinib • Klinische karakteristieken

28

Farmacogenetica sunitinib effectiviteit

29

Kiemcel versus Somatische mutaties: Cetuximab

k-ras wild type

mutant

growth-signals 30

Karapetis, N Engl J Med 2008;359(17):1757-65

Cairo-2 studie • Multicenter DCCG studie eerstelijns behandeling gemetastaseerd colorectaal carcinoom (mCRC) – PI: Prof. C.J.A. Punt, UMC St. Radboud, Nijmegen • Toevoeging cetuximab aan capecitabine + oxaliplatin + bevacizumab (Tol et al. NEJM 2009) • Blood samples: 564 van de 732 patienten • Doel: farmacogenetische markers voor cetuximab effictiviteit

31

FCGR3A 818A>C (Phe158>val) Median PFS (mo; 95% CI): Phe/Phe = 12.1 (10.3-13.2) Val-allele carrier = 7.8 (7.2-9.4) (P = 0.003, log rank test)

32

Pander, Eur J Cancer 2010 (in press)

FCGR3A 818A>C plus KRAS status Median PFS (mo): KRAS WT AC+CC AA p KRAS MT AC+CC AA p

33

Conclusies • Targeted therapies vertonen variabele respons • Variabiliteit • Farmacokinetiek • Farmacodynamiek • Niet-genetische determinanten

• Exploratieve farmacogenetische associatiestudies • Transporters en metabolisme • ‘Drug targets’

• (Nog) geen toepassing in kliniek

34

=8.2 =12.8 =0.025 =7.8 =12.1 =0.006

Dank aan

Dr Hans Gelderblom

Dr Nielka van Erp

Dr Tahar van der Straaten Laboratory for Experimental and Clinical Pharmacogenetics

Dr Judith Wessels 35