SPT with peach commercial extract (Lofarma, Milan, Italy, containing 40mcg/ml LTP) was performed on two separate occasions with 10 months interval, and they showed mean wheals diameters of 2mm. PP performed with peach fruit juice (Jolly Colombani, containing about 50% of pulp and 1% of peel) and with nectarine (pulp and peel) showed mean wheal diameters of 2 and 3mm, respectively. Values of seric specific IgE (ImmunoCAP, Phadia, Uppsala, Sweden) scored as follows: peach=0.10kUA/L, apple and apricot=0.00kUA/L, cherry=0.03kUA/L, and plum=0.01kUA/L. Molecular allergologic test (microarray ImmunoCAP ISAC 103, Phadia, Uppsala, Sweden) resulted positive for Fel d 1 (0.17kUA/L), Cri j 1 (0.95kUA/L) and Cup a 1 (18.32kUA/L). All the rest tested by ISAC resulted negative, in particular IgE specific for Pru p 3, Pru p 1, Mal d 1, Bet v 1, Bet v 2, and Bet v 4 were not detected.

We performed oral food challenge (OFC) followed by physical exercise test on two occasions. Both times, during the 24h preceding the test, the patient had eaten as usual (pasta, meat, vegetables, bread, milk, fish, eggs) and in particular he had not been given high fat content meals or alcohol. The patient's pulmonary function tests before OFC were normal on both occasions. Our patient underwent an OFC ingesting 400ml of peach fruit juice (Jolly Colombani, 50% of fruit, 1% of peel) and then an exercise challenge test was performed the first time (step-test, to go up one step of 30cm 30 times per minute for 10min) with no adverse reactions. The second OFC followed by exercise test was performed nine months later. The boy ingested two nectarines with peel and, immediately after exercise, the boy experienced a generalised adverse reaction characterised by bilateral ocular oedema and hyperaemia, ocular and nasal itching, nasal obstruction, rhinorrhoea and sneezing, throat constriction, dyspnoea and mild wheezing (FEV1=87%). The blood pressure was 135/68mmHg.

During the second OFC, before nectarines ingestion, our patient underwent blood tryptase analysis, which resulted negative (1.91mcg/L, n. v.<9.8mcg/L). The test was repeated 2h after onset of symptoms, and resulted again negative (2.39mcg/L).

The following March, ELISA and Immunoblot analysis (using peach extract, natural LPT of yellow peach and recombinant LTP as substrate) were performed on serum taken and stored during previous – the second one – OFC, and they both resulted negative. It was not possible to test nectarine natural extract, because we did not have this fruit when ELISA and Immunoblot were performed.

We presented a clinical case of sensitisation to nectarine characterised by suggestive history, positive OFC, weakly positive SPT but negative in vitro findings. We believe that this condition is unusual, because, in according to clinical signs experienced, we would have expected to find both clearly positive SPT and in vitro findings.

To find low levels of specific IgE in children with FDEIA is reported in literature.1 It is also reported that there are food protein specific characteristics thought to increase their potential allergenicity (the abundance of the protein in the food, multiple and linear IgE-binding epitopes, resistance of the protein to digestion and processing, and allergen structure).5 One or more of these characteristics may be enhanced or up-regulated during exercise, with the result that a state of tolerance to the food is temporarily lost, even in the presence of very low levels of specific IgE. This may justify the low values of specific serum IgE to peach and the low value of the average diameter of the wheal evoked by SPT with extracts and fresh food in our patient. Our experience suggests that, in children with FDEIA, low level of specific IgE should be considered positive. However, the absence of detectable Pru p 3 specific IgE by ISAC 103, ELISA and Immunoblot was unexpected. This suggests the possibility that these tests do not have sufficient sensitivity to detect low level of specific IgE. It is also possible that nectarine has an allergen that is not present in the yellow peach. If so, however, it remains unclear why peach PP resulted – although weakly – positive, and why the same happened with measurements of peach serum specific IgE. Moreover, the negative result of Immunoblot analysis did not allow us to further investigate the real nature of the relevant allergen protein.

We did not observe tryptase increase after the anaphylaxis experienced with nectarine OFC. In a study performed on children undergoing OFC,6 high tryptase levels had an anaphylaxis sensitivity of 89% and specificity of 88%. This sensitivity level may be insufficient and explain the normal levels of tryptase of our case.

Another interesting aspect of our case is the presence of a negative OFC with peach fruit juice. LTP are more concentrated in peel than in pulp of fruit.7 Tolerance to peach fruit juice of our patient could be explained by the fact that the percentage of peel contained inside fruit juice is low.

One previous study8 reported a paediatric case of FDEIA induced by Rosaceae fruits characterised by a discrepancy between positive clinical history (two episodes of FDEIA during intense exercise after eating Rosaceae fruits) and positive SPT (peach extract=4mm, peach pulp=6mm, peach peel=2mm), versus negative in vitro findings (Pru p 3, Pru p 1, Bet v 1, Bet v 2, and Bet v 4 scored negative). Authors suggested the possibility that the patient reacted to a different peach allergen or, alternatively, that he recognised a LTP isoform different from that in UniCAP.

Bianchi et al.8 did not consider appropriate to perform an OFC followed by exercise challenge test, but our case, in which diagnosis of FDEIA by nectarine was confirmed only by OFC followed by physical exercise, shows that sensitivity of molecular diagnostic tests performed by ISAC 103 is not optimal, as also Bianchi et al. said,8 and that, if clinical history is suggestive of food sensitisation, it is better to first carry out PP with natural suspected food, and eventually to perform OFC followed by exercise test.

Our conclusion is that OFC followed by exercise challenge test can be useful in children with suggestive clinical history for food sensitisation, as ISAC 103 molecular diagnostic tests sensitivity does not seem to always be optimal.

The authors have no conflict of interest to declare.