The research advances and the clinical value of antibody-drug conjugate from molecular subtyping of breast cancer in the era of

doi:10.19401/j.cnki.1007-3639.2023.12.002

Abstract

Abstract:

The incidence of breast cancer currently ranks first among malignant tumors in women. Breast cancer exhibits high heterogeneity and can be classified into four molecular subtypes: luminal A, luminal B, human epidermal growth factor receptor 2 (HER2) overexpression and triple-negative. However, previous molecular subtype classifications have limited treatment options for patients with HER2 low expression. In recent years, with the rapid development of antibody-drug conjugates (ADCs), new treatment options have emerged for breast cancer patients with HER2 low expression. This has also led to updates in the criteria for determining HER2 expression status in both domestic and international guidelines, based on immunohistochemistry (IHC) and in situ hybridization (ISH) testing, categorizing HER2 expression as HER2-positive (IHC 3+ or IHC 2+/ISH+), HER2 low expression (IHC 1+ or IHC 2+/ISH-),and HER2-negative (IHC 0). ADCs are immunotherapeutics composed of a linker that conjugates a monoclonal antibody with a cytotoxic payload. In the field of breast cancer, several large clinical trials have demonstrated clinical benefits of ADCs targeting HER2, such as trastuzumab emtansine (T-DM1), trastuzumab deruxtecan (T-DXd) and sacituzumab govitecan targeting trophoblast cell surface antigen 2 (TROP2), in various molecular subtypes of breast cancer. With the phase Ⅲ DESTINY-Breast03 trial and others, T-DXd has been found to have superior efficacy compared to T-DM1 in advanced HER2-positive breast cancer patients (approximately two times higher complete response rate, and four times longer median progression-free survival). T-DXd has now replaced T-DM1 as the recommended second-line therapy for HER2-positive breast cancer and as a second-line treatment option after local treatment for brain metastasis. The phase Ⅲ DESTINY-Breast04 trial confirmed that breast cancer patients with HER2 low expression can also benefit from T-DXd, further reshaping the treatment landscape for advanced breast cancer and supporting the need to redefine molecular subtypes of HER2-negative breast cancer. The phase Ⅲ ASCENT trial demonstrated that sacituzumab govitecan significantly improved survival and quality of life in triple-negative breast cancer (TNBC) patients, and the phase Ⅱ NeoSTAR study suggested its potential as neoadjuvant therapy in TNBC. Based on evidence, T-DM1, T-DXd and sacituzumab govitecan have been approved for marketing in both foreign and Chinese markets. Other ADC drugs, such as HER3-DXd, Dato-DXd and China-developed RC48, are also undergoing extensive clinical trials in the field of breast cancer and other tumors. Furthermore, there are several other ADCs targeting different molecular targets in active development. This article aimed to review the new advances related to ADCs therapy for breast cancer patients with different molecular subtypes and discuss the clinical application value of ADCs in breast cancer.

Key words: Breast cancer, Molecular typing, Human epidermal growth factor receptor 2, Antibody-drug conjugate

CLC Number:

R737.9

WANG Xueer, WANG Yongsheng. The research advances and the clinical value of antibody-drug conjugate from molecular subtyping of breast cancer in the era of "precision medicine"[J]. China Oncology, 2023, 33(12): 1073-1082.

Figures/Tables 2

Tab. 1

Tab. 2

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Study drug	Study name	Clinical staging	HER2 status of study population	Treatment protocol/ number of lines	Primary efficacy endpoint	Safety
T-DXd	DESTINY-Breast01^[13]	Phase Ⅱ	Positive HER2	T-DXd Second-line and late-line therapy	ORR: 60.9%	AE: 99.5% ≥Grade 3 AE: 57.1%
	DESTINY-Breast02^[46]	Phase Ⅲ		T-DXd vs capecitabine + trastuzumab/lapatinib selected by clinicians Third-line therapy	Median PFS evaluated by BICR: 17.8 months vs 6.9 months (P<0.000)	TEAE: >99% vs 95% ≥Grade 3 TEAE: 53% vs 44%
	DESTINY-Breast03^[16]	Phase Ⅲ		T-DXd vs TDM1 Second-line and late-line therapy	Median PFS evaluated by BICR: 28.8 months vs 6.8 months (P<0.000)	TEAE: >99% vs 95% ≥Grade 3 TEAE: 56% vs 52%
T-DXd	DESTINY-Breast04^[13]	Phase Ⅲ	Low HER2 expression	T-DXd vs routine chemotherapy Second-line and late-line therapy	Median PFS: 10.1 months vs 5.4 months	AE: 99.5% vs 98.3% ≥Grade 3 AE: 52.6% vs 67.4%
Sacituzumab govitecan	TROPiCS-02^[38]	Phase Ⅲ	Negative HER2	Ditto Third-line and late-line therapy	Median PFS evaluated by BICR: 5.5 months vs 4.0 months (P=0.001)	Important ≥Grade 3 TEAE: Neutropenia: 51% vs 38% Diarrhea: 9% vs 1%
	ASCENT^[41]	Phase Ⅲ		Sacituzumab govitecan vs capecitabine, eribulin, vinorelbine or gemcitabine selected by clinicians Third-line and post-line therapy	Median PFS evaluated by BICR PFS: 5.6 months vs 1.7 months (P<0.001)	AE: 98% vs 86% Grade 3/4 AE: 64% vs 47%

Target/study drug	Trial/study name	Clinical staging/study design	Study population	Treatment protocol	Status
HER3/patritumab deruxtecan（HER3-DXd, U3-1402）	NCT04610528/TOT-HER3	Phase Ⅰ/single group assignment	HR+/HER2- early breast cancer	U3-1402	Active, not recruiting
Nectin4/enfortumab vedotin（EV, ASG-22CE）	NCT04225117/EV-202	Phase Ⅱ/parallel assignment	Locally advanced or metastatic malignant solid tumors (including HR+/HER2- breast cancer; TNBC)	ASG-22CE	Active, not recruiting
LIV-1/ladiratuzumab vedotin（SGN-LIV1A）	NCT03310957	Phase Ⅰb, Ⅱ/single group Assignment	TNBC	SGN-LIV1A + pembrolizumab	Active, not recruiting
ROR2/CAB-ROR2-ADC (BA3021)	NCT03504488	Phase Ⅰ, Ⅱ/RCT	Solid tumors (including TNBC)	BA3021 vs BA3021 + PD-1 inhibitor	Recruiting
TROP2/datopotamab deruxtecan (Dato-DXd)	NCT05460273/TROPION-PanTumor02	Phase Ⅰ, Ⅱ/single group assignment	TNBC; NSCLC	Dato-DXd	Active, not recruiting
TROP2/SKB264	NCT04152499	Phase Ⅰ, Ⅱ/sequential assignment	Advanced unresectable/metastatic solid tumors (including HR+/HER2- breast cancer; TNBC)	SKB264	Recruiting
Tubulin tissue factor/XB-002	NCT04925284/JEWEL-101	Phase Ⅰ/RCT	Advanced solid tumors (including HR+ breast cancer, TNBC)	XB-002 ± nivolumab/bevacizumab	Recruiting
FRɑ/farletuzumab ecteribulin	NCT04300556	Phase Ⅰ, Ⅱ/sequential assignment	Solid tumor (including TNBC)	Farletuzumab ecteribulin	Recruiting