Screening for F508del as a first step in the molecular diagnosis of cystic fibrosis

Marson, Fernando Augusto de Lima; Bertuzzo, Carmen Silvia; Ribeiro, Maria Ângela Gonçalves de Oliveira; Ribeiro, Antônio Fernando; Ribeiro, José Dirceu

doi:10.1590/S1806-37132013000300007

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Jornal Brasileiro de Pneumologia

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ORIGINAL ARTICLES • J. bras. pneumol. 39 (3) • June 2013 • https://doi.org/10.1590/S1806-37132013000300007 copy

Screening for F508del as a first step in the molecular diagnosis of cystic fibrosis^* * Study carried out in the Department of Pediatrics, in the Molecular Genetics Laboratory, and in the Pulmonary Physiology Laboratory of the Center for Pediatric Studies, State University at Campinas School of Medical Sciences, Campinas, Brazil. ^ A versão completa em português deste artigo está disponível em www.jornaldepneumologia.com.br

Authorship SCIMAGO INSTITUTIONS RANKINGS

OBJECTIVE:

To determine the relevance of screening for the F508del mutation of the cystic fibrosis transmembrane conductance regulator gene as a first step in the genetic diagnosis of cystic fibrosis (CF) by associating the genotype with various clinical variables.

METHODS:

We evaluated 180 CF patients regarding the F508del mutation. The clinical data were obtained from the medical records of the patients and from interviews with their parents or legal guardians.

RESULTS:

Of the 180 patients studied, 65 (36.1%) did not carry the F508del mutation (group 0 [G0]), 67 (37.2%) were F508del heterozygous (G1), and 48 (26.7%) were F508del homozygous (G2). All three groups showed associations with the clinical variables. Homozygosis was associated with younger patients, younger age at CF diagnosis, and younger age at the first isolation of Pseudomonas aeruginosa (PA), as well as with higher prevalence of pancreatic insufficiency (PI) and non-mucoid PA (NMPA) colonization. In comparison with G1+G2 patients, G0 patients were older; first experienced clinical symptoms, digestive disease, and pulmonary disease at an older age; were older at CF diagnosis and at first PA isolation; and had a lower prevalence of PI and meconium ileus, as well as of colonization by NMPA, mucoid PA, and Burkholderia cepacia. In G1 patients, values were intermediate for age at CF diagnosis; age at first PA isolation, first pulmonary symptoms, and first clinical manifestations; MPA colonization; and OR for PI.

CONCLUSIONS:

The identification of F508del in 63.9% of the patients studied showed that this can be a useful tool as a first step in the genetic diagnosis of CF. The F508del genotype was associated with clinical severity of the disease, especially with the variables related to CF onset.

Cystic Fibrosis; Cystic Fibrosis Transmembrane Conductance Regulator; Genotype; Mutation

Variable		Result
Males		50.00
Age, years		17.72 ± 15.75 (0.60-24.00)
Caucasoid		91.70
Underweight and extremely underweight		22.47
Identification of one F508del allele		37.20
Identification of two F508del alleles		26.70
Age at first clinical manifestations, years		2.90 ± 8.88 (0.00-13.00)
Age at diagnosis, years		7.62 ± 13.63 (0.00-14.23)
Age at first digestive symptoms, years		3.39 ± 9.11 (0.00-12.45)
Age at pulmonary symptoms, years		2.90 ± 9.89 (0.00-13.00)
SaO₂, %		94.92 ± 4.26 (66.00-99.00)
Bhalla score		8.74 ± 5.72 (0.00-25.00)
Kanga score		18.85 ± 5.84 (10.00-40.00)
Shwachman-Kulczycki score		65.85 ± 16.77 (20.00-95.00)
FVC, % of predicted		79.29 ± 23.55 (19.00-135.00)
FEV₁, % of predicted		71.29 ± 27.47 (17.00-132.00)
FEV₁/FVC, % of predicted		83.46 ± 15.95 (37.00-137.00)
FEF_25-75%		59.05 ± 35.55 (7.00-150.00)
Nasal polyps		18.64
Diabetes mellitus		18.64
Osteoporosis		16.38
Pancreatic insufficiency		79.90
Meconium ileus		15.08
Age at first isolation of Pseudomonas aeruginosa, years		8.55 ± 14.45 (2.00-15.00)
Colonization^b
	P. aeruginosa	56.42
	Mucoid P. aeruginosa	42.46
	Burkholderia cepacia	13.97
	Achromobacter xylosoxidans	10.05
	Staphylococcus aureus	78.77

		Patient
F508del mutation group	CFTR mutation genotype	n	%	% per group
G0	-/-	43	23.9	36.1
	G542X/-	5	2.8
	G542X/R1162X	1	0.6
	G542X/I618T	1	0.6
	G542X/2183A>G	1	0.6
	G542X/2183AA→G	1	0.6
	G542X/P205S	1	0.6
	G542X/R334W	1	0.6
	I507V/-	1	0.6
	R334W/R1066C	1	0.6
	R334W/R334W	1	0.6
	3120+1G>A/3120+1G>A	1	0.6
	3120+1G>A/-	1	0.6
	TG11-5T/-	1	0.6
	622-2A>G/711+1G>T	1	0.6
	R1162X/R1162X	1	0.6
	R1162X/-	1	0.6
	D110H/V232H	1	0.6
G1	F508del/-	40	22.2	37.2
	F508del/G542X	13	7.2
	F508del/R1162X	5	2.8
	F508del/N1303K	4	2.2
	F508del/R553X	2	1.1
	F508del/S4X	1	0.6
	F508del/1717-1G>A	1	0.6
	F508del/exon 6B-16 duplication	1	0.6
	F508del/2184insA	1	0.6
G2	F508del/F508del	48	26.7	26.7

Variable	Genotype group	Median	Mean	SD	p
Shwachman-Kulczycki score	G0	95	93.38	5.935	0.046
Shwachman-Kulczycki score	G1+G2	96	95.50	2.869	0.046
SaO₂	G0	60	61.40	17.844	0.034
SaO₂	G1+G2	65	67.91	15.893	0.034

Group	Variable	Categorization		p	OR	95% CI	Variable	Categorization		p	OR	95% CI
	Age	≤ 154 mo	> 154 mo				Age at first clinical manifestations	≤ 3 mo	> 3 mo
G0		18	46	< 0.001	0.238	0.121-0.457		19	37	< 0.001	0.239	0.119-0.47
G1		36	31		1.202	0.654-2.217		48	18		2.974	1.539-5.884
G2		37	11		4.754	2.263-10.53		30	18		1.366	0.689-2.749
	Age at diagnosis	≤ 24 mo	> 24 mo				Age at digestive disease	≤ 3 mo	>3 mo
G0		15	44	< 0.001	0.157	0.007-0.315		13	27	0.023	0.362	0.165-0.77
G1		41	23		1.95	1.034-3.725		37	25		1.852	0.958-3.615
G2		36	12		3.563	1.715-7.74		26	22		1.227	0.615-2.464
	Age at pulmonary disease	≤ 6 mo	> 6 mo				PI	Presence	Absence
G0		20	32	0.006	0.385	0.179-0.704		35	29	< 0.001	0.08	0.03-0.192
G1		44	21		2.258	1.181-4.391		62	5		4.71	1.817-14.35
G2		28	20		1.158	0.586-2.312		46	2		7.007	2.136-51.37
	MI	Presence	Absence				Age at first PA isolate	≤ 3 mo	> 3 mo
G0		5	60	0.047	0.335	0.108-0.892		9	26	0.001	0.229	0.093-0.535
G1		13	54		1.569	0.683-3.576		30	25		1.263	0.627-2.552
G2		10	38		1.662	0.682-3.906		28	13		2.794	1.29-6.248
	MPA	Presence	Absence				NMPA	Presence	Absence
G0		21	44	0.068	0.553	0.2731-0.984		28	37	0.025	0.438	0.233-0.814
G1		35	32		1.914	1.034-3.56		41	26		1.39	0.752-2.593
G2		20	28		0.97	0.491-1.898		32	16		1.82	0.916-3.702
	BC	Presence	Absence
G0		4	61	0.101	0.313	0.088-0.91
G1		12	55		1.83	0.757-4.426
G2		8	40		1.447	0.548-3.618

Clinical variable		Genotype	G2 vs. G0+G1	G0 vs. G1+G2
		p	p	p
Sex		0.473	0.400	1
Ethnicity		0.353	0.549	0.407
Age		< 0.001	< 0.001	< 0.001
Age at first clinical manifestations		< 0.001	0.394	< 0.001
Age at diagnosis		< 0.001	0.001	0.01
Onset of digestive symptoms		0.022	0.602	< 0.001
Onset of pulmonary symptoms		0.006	0.731	0.004
BMI		0.227	0.22	0.186
Bhalla score		0.163	0.283	0.06
Kanga score		0.509	0.466	0.264
Shwachman-Kulczycki score		0.098	0.889	0.046
SaO₂		0.068	0.076	0.034
FVC, % of predicted		0.514	0.368	0.29
FEV₁, % of predicted		0.321	0.054	0.383
FEV₁/FVC, % of predicted		0.49	0.232	0.596
FEF_25-75%		0.29	0.27	0.132
Nasal polyposis		0.521	0.516	0.842
Diabetes mellitus		0.948	1	0.842
Osteoporosis		0.236	0.255	0.139
Pancreatic insufficiency		< 0.001	0.001	< 0.001
Meconium ileus		0.047	0.238	0.016
	First isolation of Pseudomonas aeruginosa	0.001	0.009	0.001
Colonization
	P. aeruginosa	0.025	0.092	0.012
	Mucoid P. aeruginosa	0.068	1	0.059
	Burkholderia cepacia	0.332	0.46	0.04
	Achromobacter xylosoxidans	0.101	0.261	0.301
	Staphylococcus aureus	0.758	1	0.572

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E-mail: jbp@sbpt.org.br

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[1] Correspondence to: Fernando Augusto de Lima Marson Department of Pediatrics, State University at Campinas School of Medical Sciences CEP 13081-970, P.O. Box: 6111, Campinas, SP, Brasil Tel. 55 19 3521-8902 E-mail: fernandolimamarson@hotmail.com