ESMO Asia Congress 2022

Abstract 153P

Background

mUC is an aggressive disease with limited overall survival. HER2 overexpression is associated with poor prognosis and occurs in a significant number of patients (pts) with mUC. HER2-targeted ADCs represent a promising strategy in mUC, with multiple ongoing clinical trials. We aimed to realize a systematic review of efficacy and toxicity of anti-HER2 ADCs in mUC.

Methods

A systematic review of the literature was performed in June 2022 according to PRISMA statement. The search method included the terms bladder carcinoma or urothelial carcinoma; disitamab vedotin; HER2-targeted therapy; antibody-drug conjugate. Only prospective clinical trials were included.

Results

Ultimately, 6 phase 1 or 2 clinical trials with 236 pts were selected and 3 drugs were identified: Disatamab vedotin (DV), Trastuzumab Deruxtecan (TDXd), and MRG002. Efficacy outcomes are presented in the table. DV was tested as monotherapy in two phase 2 trials with HER2+ pts (IHC 2 or 3+); the overall response rate (ORR) ranged from 46.9 to 51.2%. Another phase 2 trial tested DV in HER2- pts, ORR was 26 % and disease control rate (DCR) was 94.7%. Preliminary results of DV combined with toripalimab as 1L in cis-ineligible pts or 2L treatment showed a RR of 76.7% and DCR of 96.7%. An ongoing trial is testing MRG002 in HER2+ pts; first results demonstrated ORR of 55% and DCR of 59%. A phase 1b is testing TDXd combined with nivolumab, the ORR was 36.7%, with a median duration of response of 13.1 months. There is a remarkable heterogeneity of HER2 positivity definition among the studies. However, subgroup analysis in all trials suggest some association between the level of HER2 expression and efficacy. TRAE occurred in 100% of included pts, incidence of G3 ranged from 15.8% to 73.5%. Most commons AE were hypoesthesia, alopecia, AST/ ALT increase and hematologic toxicity. Notably, pneumonitis occurred in 23.5% of patients treated with TDXd + nivolumab Table: 153P

Trial	Author	Drug	Year	Type	N	Phase	Age (years)	Male (%)	Disease	mFU (m)	mOS (m)	mPFS (m)	RR (%)	CR (%)	DCR (%)	DOR (m)
NCT03507166	Sheng X	Disatamab Vedotin	2021	Article	43	2	64 (45-75)	76.7	Post CT HER2 3+ / 2+	20.3	13.9	6.9	51.2	0	90.7	6.9
NCT03809013	Sheng X	2021	Abstract	64	2	62.5	NR	Post CT HER2 3+/ 2+	NR	14.8	4.3	46.9	NR	NR	8.3
NCT04264936	Zhou L	2022	Abstract	41	1b / 2	66	46.3	Plus Toripalimab 1L (cis ineligible) or post CT	8.0	NR	9.2	76.7	10	96.7	NR
NCT04073602	Xu H	2022	Abstract	19	2	64	NR	HER2 negative (IHC 0 or 1+)	NR	16.4	5.5	26.3	0	94.7	4.3
DS8201-A-U105 cohort 3 NCT03523572	Galsky T	Trastuzumab Deruxtecan	2022	Abstract	30	1b	70.9 (41.4-80.5)	88.2	Plus Nivolumab Post CT HER2 1+, 2+, 3+	NR	11.0	6.9	36.7	13.3	NR	13.1
NCT04839510	Qu W	MRG002	2022	Abstract	43	2	NR	NR	Post CT (HER2+)	NR	NR	5.8	55	8	89	NR

Conclusions

HER2-targeted ADCs are associated with high response rates in the treatment of mUC, including responses in HER2- pts. DV received FDA breakthrough therapy designation in 2020 for 2L treatment of HER2+ mUC. Confirmatory trials and better biomarker-based patient selection are needed.

Poster viewing 03

153P - Efficacy and toxicity of HER2-targeted antibody-drug conjugates (ADCs) in the treatment of metastatic urothelial cancer (mUC): A systematic review

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Abstract 153P

Background

Methods

Results

Conclusions

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

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Abstract 153P

Background

Methods

Results

Conclusions

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Funding

Disclosure

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