Diagnostic prediction model for levodopa-induced dyskinesia in Parkinson’s disease

SANTOS-LOBATO, Bruno Lopes; SCHUMACHER-SCHUH, Artur F.; RIEDER, Carlos R. M.; HUTZ, Mara H.; BORGES, Vanderci; FERRAZ, Henrique Ballalai; MATA, Ignacio F.; ZABETIAN, Cyrus P.; TUMAS, Vitor

doi:10.1590/0004-282X20190191

Bruno Lopes SANTOS-LOBATO

Universidade de São Paulo, Faculdade de Medicina de Ribeirão Preto, Departamento de Neurociências e Ciências Comportamentais, Ribeirão Preto SP, Brazil.

Universidade de São Paulo, Núcleo de Apoio à Pesquisa em Neurociência Aplicada, São Paulo SP, Brazil.

http://orcid.org/0000-0001-9321-5710

Artur F. SCHUMACHER-SCHUH

Hospital de Clínicas de Porto Alegre, Porto Alegre RS, Brazil.

http://orcid.org/0000-0002-8722-0908

Carlos R. M. RIEDER

Hospital de Clínicas de Porto Alegre, Porto Alegre RS, Brazil.

http://orcid.org/0000-0003-2950-7211

Mara H. HUTZ

Universidade Federal do Rio Grande do Sul, Departamento de Genética, Porto Alegre RS, Brazil.

http://orcid.org/0000-0002-9146-1229

Vanderci BORGES

Universidade Federal de São Paulo, Departamento de Neurologia, São Paulo SP, Brazil.

http://orcid.org/0000-0002-8723-2757

Henrique Ballalai FERRAZ

Universidade Federal de São Paulo, Departamento de Neurologia, São Paulo SP, Brazil.

http://orcid.org/0000-0002-3821-1407

Ignacio F. MATA

Veterans Affairs Puget Sound Health Care System, Seattle, WA, USA.

University of Washington, Department of Neurology, Seattle, WA, USA.

http://orcid.org/0000-0003-1198-0633

Cyrus P. ZABETIAN

Veterans Affairs Puget Sound Health Care System, Seattle, WA, USA.

University of Washington, Department of Neurology, Seattle, WA, USA.

http://orcid.org/0000-0002-7739-4306

Vitor TUMAS

Universidade de São Paulo, Faculdade de Medicina de Ribeirão Preto, Departamento de Neurociências e Ciências Comportamentais, Ribeirão Preto SP, Brazil.

Universidade de São Paulo, Núcleo de Apoio à Pesquisa em Neurociência Aplicada, São Paulo SP, Brazil.

http://orcid.org/0000-0003-2402-2709

Correspondence: Vitor Tumas; Departamento de Neurociências e Ciências Comportamentais, FMRP/USP; Av. Bandeirantes 3900; 14049-900 Ribeirão Preto SP, Brazil; E-mail: tumasv@rnp.fmrp.usp.br

Conflict of interest: Dr. Santos-Lobato declares no conflicts of interest; Dr. Schumacher-Schuh declares no conflicts of interest; Dr. Rieder received grant from Brazilian National Council for Scientific and Technological Development; Dr. Hutz declares no conflicts of interest; Dr. Borges received honoraria from UCB Pharma; Dr. Ferraz serves on Advisory Boards for Teva Brasil, UCB Biopharma, Roche, Zambon and receives royalties from Roche, Teva Brasil and UCB Biopharma; Dr. Mata received grants from Parkinson’s Foundation and from American Parkinson’s Disease Association; Dr. Zabetian received grants from the National Institute of Health, Department of Veteran Affairs and the American Parkinson’s Disease Association (U.S.A.); Dr. Tumas received honoraria from Teva Brasil, UCB Biopharma and Ipsen, and travel support for medical conferences from Roche.

General characteristics	Overall (n=430)	With dyskinesia (n=198)	Without dyskinesia (n=232)	p-value
Male, % (n)	55.1 (237)	52 (103)	57.8 (134)	0.24^a
Sample location (city), % (n)				0.55^a
Ribeirão Preto	30.5 (131)	32.8 (65)	28.4 (66)
São Paulo	15.3 (66)	15.7 (31)	15.1 (35)
Porto Alegre	54.2 (233)	51.5 (102)	56.5 (131)
Age at onset of PD^b	56 (46‒65)	50 (42‒59)	60 (51‒69)	<0.001^c
Age at the time of evaluation^b	65 (56‒74)	62.5 (54‒69)	67 (59‒75)	<0.001^c
Disease duration (years)^b	8 (5‒12)	11 (7‒15)	6 (4‒10)	<0.001^c
Levodopa therapy duration (years)^b	6 (3‒10)	8 (6‒12)	4 (2-6)	<0.001^c
Levodopa dose at evaluation (mg/day)^b	600 (400‒800)	700 (500‒975)	500 (300‒750)	<0.001^c
Levodopa equivalent daily dose (mg/day)^b	750 (500‒1000)	900 (634‒1180)	600 (400‒800)	<0.001^c
MDS-UPDRS Part III^b	35 (24‒50)	34 (23‒47)	38 (26‒51)	0.44^c
Tremor as initial motor symptom, % (n)	69.5 (285)	58.5 (107)	78.4 (178)	<0.001^a
Tremor dominant phenotype at evaluation, % (n)	53.8 (222)	33.5 (63)	70.7 (159)	<0.001^a
Hoehn & Yahr stage, % (n)				0.003^a
1	4.2 (18)	1 (2)	6.9 (16)
2	63.8 (272)	61.5 (120)	65.8 (152)
3	20.7 (88)	25.1 (49)	16.9 (39)
4	8.7 (37)	8.2 (16)	9.1 (21)
5	2.6 (11)	4.1 (8)	1.3 (3)
Use of dopaminergic agonists, % (n)	35.6 (151)	46.9 (92)	25.9 (59)	<0.001^a
Use of amantadine, % (n)	27.1 (114)	43.8 (84)	13.2 (30)	<0.001^a
Use of MAO-B inhibitors, % (n)	5.5 (23)	6.3 (12)	4.8 (11)	0.52^a
Use of COMT inhibitors, % (n)	11.4 (48)	18.8 (36)	5.3 (12)	<0.001^a

Gene (SNP)		Overall (n=430)	PD with dyskinesia (n=198)	PD without dyskinesia (n=232)	p-value^a
COMT (rs4680)
Genotype	AA	20.6 (85)	20.3 (39)	20.8 (46)	0.34
	AG	47.5 (196)	44.3 (85)	50.2 (111)
	GG	32 (132)	35.4 (68)	29 (64)
Allele	A	43.9	42.5	45.1	0.47
	G	56	57.4	54.8
DRD2/ANKK1 (rs1800497)
Genotype	AA	6.2 (24)	7.9 (14)	4.8 (10)	0.14
	AG	38.2 (147)	41.6 (74)	35.3 (73)
	GG	55.6 (214)	50.6 (90)	59.9 (124)
Allele	A	27.2	28.2	26.1	0.54
	G	72.7	71.7	73.8
DRD3 (rs6280)
Genotype	CC	29.2 (119)	24.9 (47)	32.9 (72)	0.2
	CT	48.8 (199)	51.9 (98)	46.1 (101)
	TT	22.1 (90)	23.3 (44)	21 (46)
Allele	C	53.4	50.8	55.8	0.17
	T	46.5	49.1	44.1
DAT1 (rs393795)
Genotype	TT	4.7 (8)	4.5 (4)	4.9 (4)	0.78
	TG	31.2 (53)	29.5 (26)	32.9 (27)
	GG	64.1 (109)	65.9 (58)	62.2 (51)
Allele	T	20.2	19.3	21.3	0.68
	G	79.7	80.6	78.6
MAOB (rs1799836)^b
Genotype	Female
	CC	25.7 (48)	24.5 (23)	26.9 (25)	0.13
	CT	49.7 (93)	44.7 (42)	54.8 (51)
	TT	24.6 (46)	30.9 (29)	18.3 (17)
	Male
	C	57.3 (130)	52.5 (52)	60.9 (78)	0.2
	T	42.7 (97)	47.5 (47)	39.1 (50)
Allele (Female)	C	49.7	46.2	53.2	0.21
	T	50.2	53.7	46.7
BDNF (rs6265)
Genotype	CC	67.7 (266)	67.6 (121)	67.8 (145)	0.94
	CT	28.8 (113)	28.5 (51)	29 (62)
	TT	3.6 (14)	3.9 (7)	3.3 (7)
Allele	C	82	81.5	82.5	0.77
	T	17.9	18.4	17.4
ADORA2A (rs2298383)
Genotype	CC	25.7 (106)	32.3 (62)	19.9 (44)	0.01
	CT	49.9 (206)	45.3 (87)	53.8 (119)
	TT	24.5 (101)	22.4 (43)	26.2 (58)
Allele	C	50.5	54.4	46.8	0.03
	T	49.4	45.5	53.1

	Univariate analysis				Multivariate analysis
	B	OR	95%CI	p-value	B	aOR	95%CI	p-value
Clinical variables
Sex
Female	Ref				-	-	-	-
Male	-0.232	0.79	0.54‒1.16	0.23	-	-	-	-
Sample location (city)
Ribeirão Preto	Ref				-	-	-	-
São Paulo	-0.106	0.89	0.49‒1.62	0.89	-	-	-	-
Porto Alegre	-0.235	0.79	0.51‒1.21	0.28	-	-	-	-
Age at onset of PD	-0.059	0.94	0.92‒0.95	<0.0001*	-0.019	0.98	0.96‒1.00	0.08
Disease duration	0.203	1.22	1.16‒1.28	<0.0001*	0.2	1.22	1.15‒1.29	<0.0001
Levodopa dose at evaluation	0.002	1.00	1.00‒1.00	<0.0001	-	-	-	-
MDS-UPDRS Part III	-0.003	0.99	0.98‒1.00	0.57	-	-	-	-
Initial motor symptom
Other symptoms	Ref				Ref
Tremor	-0.94	0.38	0.25‒0.59	<0.0001*	-1.177	0.3	0.18‒0.51	<0.0001
Clinical motor phenotype
Postural instability with gait disorder or indeterminate	Ref
Tremor dominant	-1.564	0.20	0.13‒0.31	<0.0001	-	-	-	-
Hoehn & Yahr stage	0.32	1.37	1.08‒1.75	0.009*	-	-	-	-
Use of dopaminergic agonists	0.93	2.53	1.68‒3.81	0.009*	0.522	1.68	1.00‒2.83	0.04
Polymorphisms
COMT (rs4680)
Genotype GG	Ref
Genotype GA	-0.328	0.72	0.46‒1.12	0.14	-	-	-	-
Genotype AA	-0.226	0.79	0.46‒1.37	0.41	-	-	-	-
DRD2/ANKK1 (rs1800497)
Genotype GG	Ref
Genotype GA	0.334	1.39	0.91‒2.13	0.12	-	-	-	-
Genotype AA	0.657	1.92	0.82‒4.53	0.13	-	-	-	-
DRD3 (rs6280)
Genotype TT	Ref
Genotype TC	0.014	1.01	0.61‒1.66	0.95	-	-	-	-
Genotype CC	-0.382	0.68	0.39‒1.18	0.17	-	-	-	-
DAT1 (rs393795)
Genotype GG	Ref
Genotype GT	-0.119	0.88	0.47‒1.66	0.71	-	-	-	-
Genotype TT	-0.423	0.65	0.17‒2.44	0.52	-	-	-	-
MAOB (rs1799836)
Genotype CC (Females)	Ref
Genotype CT (Females)	-0.111	0.89	0.44‒1.79	0.75	-	-	-	-
Genotype TT (Females)	0.617	1.85	0.81‒4.22	0.14	-	-	-	-
Genotype CC (Males)	Ref
Genotype TT (Males)	0.344	1.41	0.82‒2.39	0.2	-	-	-	-
BDNF (rs6265)
Genotype CC	Ref
Genotype CT	-0.014	0.98	0.63‒1.53	0.94	-	-	-	-
Genotype TT	0.181	1.19	0.4‒3.51	0.74	-	-	-	-
ADORA2A (rs2298383)
Genotype TT	Ref				Ref
Genotype TC	-0.014	0.98	0.6‒1.59	0.95	0.166	1.18	0.65‒2.13	0.58
Genotype CC	0.642	1.9	1.09‒3.3	0.02*	0.903	2.46	1.26‒4.82	0.008

	Clinical prediction model				Mixed prediction model
	B	OR	BCa 95% CI	p-value	B	OR	BCa 95%CI	p-value
Age at onset of PD	-0.019	0.98	-0.04-0.002	0.08	-0.032	0.96	-0.05--0.01	0.003
Disease duration	0.206	1.22	0.14-0.29	0.001	0.198	1.21	0.13-0.28	0.001
Use of dopaminergic agonists	0.543	1.72	0.05-1.08	0.034	-	-	-	-
Initial motor symptom	-1.17	0.31	-1.66--0.67	0.001	-1.229	0.29	-1.79--0.74	0.001
ADORA2A SNP (rs2298383)	-	-	-	-	0.825	2.28	0.28-1.41	0.006
Intercept	-0.439	0.64	-	0.58	0.425	1.53	-	0.56

P r e d i c t e d p r o b a b i l i t y o f L I D = \frac{e x p (a g e a t o n s e t o f P D \times - 0.019 + d i s e a s e d u r a t i o n \times 0.206 +}{\begin{matrix} 1 + e x p (a g e a t o n s e t o f P D \times - 0.019 + d i s e a s e d u r a t i o n \times 0.206 + \\ \frac{u s e o f d o p a m i n e r g i c a g o n i s t \times 0.543 + t r e m o r a s i n i t i a l m o t o r s y m p t o m \times - 1.17 + - 0.439)}{u s e o f d o p a m i n e r g i c a g o n i s t \times 0.543 + t r e m o r a s i n i t i a l m o t o r s y m p t o m \times - 1.17 + - 0.439)} \end{matrix}}

P r e d i c t e d p r o b a b i l i t y o f L I D = \frac{e x p (a g e a t o n s e t o f P D \times - 0.032 + d i s e a s e d u r a t i o n \times 0.198 +}{\begin{matrix} 1 + e x p (a g e a t o n s e t o f P D \times - 0.032 + d i s e a s e d u r a t i o n \times 0.198 + \\ \frac{t r e m o r a s i n i t i a l m o t o r s y m p t o m \times - 1.229 + A D O R A 2 A C C g e n o t y p e \times 0.825 + 0.425)}{t r e m o r a s i n i t i a l m o t o r s y m p t o m \times - 1.229 + A D O R A 2 A C C g e n o t y p e \times 0.825 + 0.425)} \end{matrix}}

[1] Correspondence: Vitor Tumas; Departamento de Neurociências e Ciências Comportamentais, FMRP/USP; Av. Bandeirantes 3900; 14049-900 Ribeirão Preto SP, Brazil; E-mail: tumasv@rnp.fmrp.usp.br

Brasil

Brasil

Diagnostic prediction model for levodopa-induced dyskinesia in Parkinson’s disease

Modelo de predição diagnóstica para discinesias induzidas por levodopa na doença de Parkinson

Abstract

Background:

Objective:

Methods:

Results:

Conclusion: