Table 3

Molecular characterisation of the CFTR rearrangements

Patient no.	Rearrangement	Simplified name	Exon(s) involved	Linked haplotype IVS1(CA)-IVS8(CA)- IVS17b(TA)-IVS17b(CA)	Motif sequence at the breakpoints
The nomenclature recommendations were followed (www.hgvs.org) but the A of the ATG translation start codon was numbered as +133, according to the current CFTR gene numbering (GenBank NM_000492.2) and the CF mutation database. The new rearrangements are indicated in bold.
*The same indel was described in a CF patient with paternal isodisomy²² and further found in a French CF patient.¹⁴
†The same CFTRdele2 as that described by Mekus and Tümmler (www.genet.sickkids.on.ca/cftr) was identified using specific primers provided by T Dörk.
‡Abnormal segregation of the IVS17b(TA) microsatellite was observed using the flanking primers,⁴² as the 3′ breakpoint is located within this site. The number of (TA) repeats, indicated in italics, has thus been determined by sequencing.
§The linked haplotype was demonstrated in case nos. 5 and 6 and hypothesised in case nos. 7 and 8.
¶The precise IVS1(CA) allele could not be determined, as the father’s DNA was not available.
**The linked haplotype was hypothesised, considering the most frequent haplotype IVS8(CA)23-IVS17b(TA)33-IVS17b(CA)13 linked to G542X.⁴³
1	c.136_c.185+69del119bpins299bp*	136del119ins299	Part of 1 (codons 2–18)	23–16–29–13	Inverted CCATG
2	c.186−?_c.296+?del†	CFTRdele2	2	24–16–30–14	ND
3	c.3413_c.3499+268del355bpins TGTTAA	3413del355ins6	Part of 17b (codons1094–1122)	23–16–del–13	Direct CTGT andAT rich
4	c.2752–674_c.3499+198del9855bp	*CFTR* dele14b–17b	14b–17b	23–16–13–13‡	Direct TCGG andAT rich
5–8	c.3121–977_c.3499+248del2515bp	*CFTR* dele17a–17b	17a–17b	23–16–7–13‡,§	Symmetric ATG andAT rich
9	[c.297−?_c.1716+?del; c.2752−?_c.3120+?del]	*CFTR* dele3–10,14b–16	3–10 and 14b–16	22 or 23–16–7–17¶	ND
10	CFTRdele1–24	*CFTR* dele1–24	1–24	del–del–del–del	ND
11	c.406−?_c.1341+?dup	*CFTR* dup4–8	4–8	27–17–7–17**	ND