Abstract 412P
Background
As is known to all, refractory pruritus is common in patients treated with targeted drug. Substance P is an important neuro-mediator of pruritus. Aprepitant is the world's first new generation of an oral neurokinin 1 receptor antagonist, which is used in combination with other antiemetics to prevent chemotherapy-induced nausea and emesis(CINV). Our previous cases have showed that pruritus caused by targeted medications have good response to aprepitant. However, there is no clinical data on relationship between substance-P in the blood and efficacy of aprepitant.
Methods
The study enrolled 36 patients with refractory pruritus induced by targeted drug. All the patients received aprepitant (day 1, 125 mg; day 2, 80 mg; day 3 80mg). Substance P was measured at baseline(D1)and 7 days later(D7). The primary endpoint was the relationship between substance-P in the blood and efficacy of aprepitant. The Visual Analogue Scale (VAS) score is used to evaluate the efficacy of aprepitant. The tocxicity was determined according to CTCAE 4.0.
Results
The patients were enrolled From Nov. 2021 to Feb. 2022. The average age was 56 years old. The PS score of 33 patients were 1 and 3 patients were 2. Only 2 patients showed no response. Other 34 patients showed superior response especially Pt3 and Pt26, the amount of substance P in the blood respectively from 10322pg/ml to 3486pg/ml and 9226pg/ml to 2717pg/ml. Among the effective patients, the average change of VAS score is 6. Pt25 showed the best change of VAS score from 10 to 0. The toxicities associated with this protocols were manageable. Only 1 patient was 3/4-grade fatigue.
Conclusions
Substance-P in the blood is well-related with the efficacy of aprepitant for targeted drug-induced refractory pruritus in chinese malignancy population. It may provide a new and effective indicator for this therapy strategy, what we do next is to explore the cut-off value of substance-P at baseline who will benefit from the aprepitant.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
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