Delving into the Latest Updates on Fam-trastuzumab deruxtecan-NXKI with Synapse

Overview

Basic Info

Drug Type

Antibody drug conjugate (ADC)

Synonyms

Fam-trastuzumab deruxtecan, T-DXd, Trastuzumab deruxtecan

+ [15]

Target

HER2 x Top I

Action

antagonists, inhibitors

Mechanism

HER2 antagonists(Receptor tyrosine-protein kinase erbB-2 antagonists), TOP1 inhibitors(DNA topoisomerase I inhibitors), ADCC(Antibody-dependent cell-mediated cytotoxicity (ADCC) effects)

Therapeutic Areas

NeoplasmsDigestive System DisordersRespiratory Diseases+ [5]

Active Indication

Stomach CancerHER2 Positive Solid TumorsHR-positive/HER2-low Breast Carcinoma+ [74]

Inactive Indication

Adenocarcinoma of LungAdvanced HER2-Positive Breast CarcinomaHER2 Positive Transitional Cell Carcinoma+ [3]

Originator Organization

Daiichi Sankyo Co., Ltd.

Active Organization

Daiichi Sankyo Co., Ltd.

AstraZeneca PLCAstraZeneca AB

+ [8]

Inactive Organization-

License Organization

Merck & Co., Inc.

AstraZeneca PLC

Daiichi Sankyo Co., Ltd.

+ [2]

Drug Highest PhaseApproved

First Approval Date

United States (20 Dec 2019),

HER2 Positive Breast Cancer

RegulationFast Track (United States), Accelerated Approval (United States), Orphan Drug (United States), Orphan Drug (Japan), Orphan Drug (Australia), Priority Review (Australia), SAKIGAKE (Japan), Breakthrough Therapy (China), Priority Review (United States), Conditional marketing approval (China), Priority Review (China), Breakthrough Therapy (United States)

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Structure/Sequence

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Sequence Code 18481L

Source: *****

Sequence Code 44772H

Source: *****

Purpose: This clinical trial is designed to evaluate the safety and effectiveness of Trastuzumab Deruxtecan for patients with HER2 Positive Newly Diagnosed Metastatic Esophageal, Gastric, GEJ Cancer. The goal is to determine how well this treatment works and to identify any potential side effects.
Who Can Participate: We are looking for Participants with histologically confirmed HER2 positive locally advanced unresectable and/or metastatic esophageal, gastric or GEJ adenocarcinoma with an ECOG PS of 2 and measurable disease according to RECIST 1.1 within 42 days prior to registration. Participants will be carefully screened to ensure they meet the study requirements.
What to Expect: Participants will undergo 6.4mg/kg, IV infusion of Trastuzumab deruxtucan over the course of the study. They will receive detailed information about the study and will have the opportunity to ask questions before deciding to participate. Informed consent will be obtained to ensure that participants understand the study's purpose, procedures, risks, and benefits.
Safety Monitoring: The health and safety of participants are our top priority. An Independent Data and Safety Monitoring Committee (DSMC) will regularly review the study data to ensure participant safety and to monitor for any adverse events. Any serious side effects will be reported and addressed promptly.
Benefits and Risks: While the study aims to provide potential benefits, such as improved treatment options for HER2 Positive Newly Diagnosed Metastatic Esophageal, Gastric, GEJ Cancer there may also be risks involved. Participants will be informed of all possible risks before enrolling in the study.
Confidentiality: All personal information will be kept confidential, and data will be used only for research purposes.
Contact Information: For more information about this study, please contact PhaseIICRA@medicine.bsd.uchicago.edu

Start Date01 Nov 2026

Sponsor / Collaborator

The University of Chicago

NCT07137416

/ RecruitingPhase 1IIT

Phase 1b Study of Pidnarulex and Trastuzumab Deruxtecan in Patients With HER2 Expressing Solid Tumors

This phase I trial tests the safety, side effects, and best dose of pidnarulex in combination with trastuzumab deruxtecan in treating patients with breast cancer and other solid tumors that express varying levels of a protein called HER2 and that has spread from where it first started (primary site) to other places in the body (metastatic), that cannot be removed by surgery (unresectable), or that has spread to nearby tissue or lymph nodes (locally advanced). Pidnarulex is an enzyme inhibitor that causes cell death and prevents tumor cell growth. Trastuzumab deruxtecan is in a class of medications called antibody-drug conjugates. It is composed of a monoclonal antibody, called trastuzumab, linked to a chemotherapy drug, called deruxtecan. Trastuzumab attaches to HER2 positive tumor cells in a targeted way and delivers deruxtecan to kill them. Giving pidnarulex in combination with trastuzumab deruxtecan may be safe, tolerable and/or effective in treating patients with metastatic, unresectable, or locally advanced HER2-expressing breast cancer or other solid tumors.

Start Date05 Oct 2026

Sponsor / Collaborator

National Cancer Institute

NCT07012031

/ RecruitingPhase 1/2IIT

A Phase I/II Study Evaluating the Safety, Tolerability, and Efficacy of Sotorasib Plus Trastuzumab Deruxtecan in Patients With Advanced Non-Small Cell Lung Cancer With a KRASG12C Mutation

This phase I/II trial tests the safety, side effects and best dose of sotorasib with trastuzumab deruxtecan and how well the combination works in treating patients with KRAS G12C mutated non-small cell lung cancer that has spread to nearby tissues or lymph nodes (locally advanced) or that has spread from where it first started (primary site) to other places in the body (metastatic). Sotorasib blocks a protein made by the mutated KRAS gene (KRAS p.G12C), which may help keep tumor cells from growing and may kill them. It is a type of targeted therapy. Trastuzumab deruxtecan is in a class of medications called antibody-drug conjugates. It is composed of a monoclonal antibody, called trastuzumab, linked to a chemotherapy drug, called deruxtecan. Trastuzumab attaches to HER2 positive tumor cells in a targeted way and delivers deruxtecan to kill them. Giving sotorasib in combination with trastuzumab deruxtecan may be safe, tolerable, and/or effective in treating patients with locally advanced or metastatic non-small cell lung cancer with a KRAS G12C mutation.

Start Date07 Aug 2026

Sponsor / Collaborator

National Cancer Institute

100 Clinical Results associated with Fam-trastuzumab deruxtecan-NXKI

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100 Translational Medicine associated with Fam-trastuzumab deruxtecan-NXKI

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100 Patents (Medical) associated with Fam-trastuzumab deruxtecan-NXKI

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1,002

Literatures (Medical) associated with Fam-trastuzumab deruxtecan-NXKI

01 Jul 2026·Value in Health Regional Issues

Budget Impact Analysis of Fam-Trastuzumab-Deruxtecan as a Second Line in Patients With HER2-Positive Metastatic Breast Cancer in Oman

Article

Author: Aljaber, Rana ; Al Froukh, Rawan F ; Al Hashar, Amna

OBJECTIVES:

Despite advancements, breast cancer remains a major global health and financial challenge. Trastuzumab-based therapies, particularly Fam-Trastuzumab-Deruxtecan (T-DXd), have shown superior outcomes, leading to its recommendation as a preferred second-line treatment. However, its high cost necessitates a budget impact analysis (BIA) to evaluate financial feasibility. This study assesses the 1-year budget impact of replacing Trastuzumab Emtansine (TDM1) with T-DXd for HER2+ metastatic breast cancer in an Omani cancer center.

METHODS:

A static BIA model was built based on National Institute for Health and Care Excellence template with adaptation as required. The model time horizon was 1 year then projected over another 2 years, using 2022 as the baseline year, adopting Omani healthcare-payer perspective. The analysis considered 2 scenarios: (1) TDM1 as the current formulary drug and (2) T-DXd is introduced instead of TDM1, assuming that treatment share would be 100%. One-way sensitivity analysis is performed to assess the model's robustness.

RESULTS:

The BIA demonstrated that replacing TDM1 with T-DXd for the eligible patients would lead to increase in the budget expenditure. Over a 3-year period, considering the provided assumptions and input data, the cumulative excess amount to €5 909 481.67. The primary contributing factors are the drug acquisition cost and the median treatment duration. The sensitivity analysis results suggest the model is robust to changes in adverse drug reaction costs, unlike changes in treatment duration and drug cost.

CONCLUSIONS:

Although T-DXd improves clinical outcomes, its adoption as a second-line treatment in Oman poses a substantial financial burden, necessitating careful budget planning to ensure long-term affordability.

01 Apr 2026·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Recent advances in systemic treatment for HER2-negative breast cancer with brain metastases

Review

Author: Zhu, Yuehong ; Hao, Chunfang ; Zhang, Jie

Human epidermal growth factor receptor 2 (HER2) -negative breast cancer brain metastases (BCBM) and leptomeningeal disease (LMD) pose significant clinical challenges due to limited treatment options and poor prognosis. Unlike HER2-positive BCBM, which has established therapeutic protocols, HER2-negative BCBM and LMD lacks standardized approaches. Recent advances have introduced novel systemic therapies targeting diverse pathways, including cell cycle regulation, DNA repair, immune modulation, vascular suppression, and leptomeningeal penetration, with emerging data supporting activity in LMD. Cyclin-dependent kinase 4/6 (CDK4/6) inhibitors show promise in hormone receptor-positive subsets, particularly when combined with radiotherapy. Antibody-drug conjugates (ADCs), such as trastuzumab deruxtecan and sacituzumab govitecan, demonstrate enhanced central nervous system penetration and tumor-specific cytotoxicity, improving outcomes in both stable and active brain metastases. Immune checkpoint inhibitors (ICIs) and poly (ADP-ribose) polymerase (PARP) inhibitors also exhibit potential, though their efficacy varies by molecular subtype. Additionally, intrathecal therapies have become a cornerstone for LMD management, bypassing the blood-CSF barrier. Emerging therapies like selective estrogen receptor degraders (SERDs) and kinase inhibitors address resistance mechanisms, offering new avenues for personalized treatment. This review underscores the need for survival-prolonging, quality-of-life-preserving strategies with optimized safety profiles, highlighting the evolving landscape of HER2-negative BCBM and LMD management.

01 Apr 2026·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Trastuzumab deruxtecan in non-breast solid tumors: Expanding indications, efficacy, and future directions

Review

Author: Petrelli, F ; Bukovec, R ; Ghidini, A ; Roncari, L ; Dottorini, L

BACKGROUND:

HER2 alterations occur across multiple malignancies beyond breast cancer, including gastric, non-small-cell lung, colorectal, gynecologic, salivary gland, biliary tract, and urothelial cancers. Trastuzumab deruxtecan (T-DXd), a next-generation antibody-drug conjugate, has transformed outcomes through its high drug-to-antibody ratio, potent topoisomerase I inhibitor payload, and membrane-permeable design enabling a bystander effect.

METHODS:

We reviewed clinical and translational evidence for T-DXd in non-breast solid tumors, focusing on efficacy, safety, biomarkers, and resistance mechanisms. Key data were derived from the DESTINY trial program, basket studies, and recent regulatory submissions.

RESULTS:

Across tumor types, T-DXd has demonstrated clinically meaningful response rates: ∼55 % in HER2-mutant NSCLC, 42-51 % in gastric cancer, 37-45 % in colorectal cancer, 57 % in endometrial cancer, and ∼60 % in salivary duct carcinoma. Durable responses have also been observed in biliary and urothelial cancers. The most frequent adverse events are gastrointestinal and hematologic, while interstitial lung disease remains the most significant toxicity, occurring in ∼10-15 % of patients, with rare fatal cases. Predictive biomarkers vary by histology: HER2 mutation is most relevant in NSCLC, whereas amplification and overexpression define benefit in gastrointestinal and gynecologic malignancies. Resistance mechanisms include HER2 downregulation, bypass signaling activation, and impaired payload release.

CONCLUSIONS:

T-DXd has emerged as a transformative therapy across HER2-driven malignancies, leading to histology-specific and tissue-agnostic approvals. Vigilant ILD monitoring is essential, and further research is warranted to refine biomarkers, address resistance, and explore rational drug combinations. T-DXd exemplifies the paradigm shift of antibody-drug conjugates toward pan-cancer precision oncology.

1,059

News (Medical) associated with Fam-trastuzumab deruxtecan-NXKI

26 Feb 2026

·endpoints.news

Voucher holder Boehringer wins sped-up approval for first-line use of lung cancer drug

The FDA greenlit an expanded label for Boehringer Ingelheim’s lung cancer drug Hernexeos, marking the first use of the Commissioner’s National Priority Voucher for a new indication. Boehringer won an accelerated approval for use of Hernexeos in advanced non-small cell lung cancer patients with certain HER2 mutations who haven’t previously been treated. In August, the agency granted accelerated approval for use of the drug in patients who have been treated with other therapies. The decision gives Boehringer an advantage over its rival Bayer, which is studying its HER2-targeted pill Hyrnuo in first-line patients. Bayer has neither received the Commissioner’s voucher nor announced an FDA submission in the first-line indication. A spokesperson for Bayer didn’t immediately respond to a request for comment. The commissioner’s voucher is a pilot program meant to significantly speed the review of drugs from “companies supporting US national interests.” Health policy experts and some former FDA officials have raised concerns over whether the program is politicizing the drug approval process. “The FDA is on the hunt for game-changing therapies that can qualify for a priority review. In this case a final decision was rendered 44 days after the filling date,” FDA Commissioner Marty Makary said in a statement on Thursday. A Boehringer spokesperson told Endpoints News in early December that it anticipated “hearing news within the coming weeks” on the Hernexeos decision. On Dec. 16, the company told Endpoints that its supplemental application “is currently under review within the parameters of this pilot program.” Last October, both Boehringer and Bayer presented data at the biggest European cancer conference, ESMO, concerning the use of their rival drugs in first-line patients. Those data showed similar efficacy, though a smaller proportion of patients who received Boehringer’s drug experienced diarrhea. About 2% to 4% of non-small cell lung cancer cases bear HER2 mutations. Boehringer and Bayer contend their drugs can provide a potentially safer and more convenient targeted treatment option for those patients compared to other HER2 therapies, such as AstraZeneca and Daiichi Sankyo’s antibody-drug conjugate Enhertu. The first commissioner’s voucher recipient to get an approval was USAntibiotics in December for Augmentin XR, an extended-release form of the antibiotic amoxicillin. GSK’s version of the antibiotic initially won US approval in 2002, but it was later pulled from the market for commercial reasons. Boehringer was one of 17 drugmakers that the Trump administration called out in July as part of its “most favored nation” push around drug pricing.

Drug ApprovalPriority ReviewAccelerated Approval

26 Feb 2026

·www.biopharmadive.com

Bristol Myers says ADC licensed from China hits mark in aggressive breast cancer

Dive Brief:Bristol Myers Squibb on Thursday touted the results of a Chinese study that showed positive results for a cancer treatment it licensed in 2023.Researchers tested the drug, iza-bren, in patients with advanced triple-negative breast cancer whose disease had progressed after previous therapy. They found that the experimental medication improved the chances of progression-free survival and overall survival, compared with chemotherapy.Sichuan Biokin, the parent company of Bristol Myers partner SystImmune, sponsored the study in mainland China. Outside of the country, Bristol Myers and SystImmune are co-developing the drug under an agreement that could potentially be worth more than $8 billion.Dive Insight:The study is another win for antibody drug conjugates, a class that has generated considerable attention among drugmakers in recent years. Bristol Myers, Merck, Pfizer, AstraZeneca, Gilead and Eli Lilly are among the major pharmaceutical companies that have inked deals to gain access to the medicines, which have spurred startups aiming to take the technology a step further.The drugs offer the promise of more targeted care for patients instead of traditional chemotherapy. The antibodies can bind to cancer cells and unleash toxins directly into them, sparing the healthy tissue that often falls victim to a blast of chemotherapy.Its an approach that has already seen great success. A leader in the class, AstraZeneca and Daiichi Sankyos Enhertu, targets HER2, a protein that is overexpressed in as much as a fifth of breast cancers. Initially approved in 2019, Enhertu is generating billions of dollars in sales and changing the way certain breast cancers are treated.Iza-bren is among a number of experimental medicines designed to improve on the basic idea of antibody drug conjugates. Instead of one target, iza-bren seeks out two, EGFR and HER3. Both are highly expressed in a range of cancers, Bristol Myers said.The Chinese study focused specifically on patients with unresectable locally advanced or metastatic triple-negative breast cancer. Bristol Myers and SystImmune are also developing the medicine for other indications, including lung cancer. And in China, two applications for the drug for nasopharyngeal carcinoma and esophageal squamous cell carcinoma have already been accepted for review.With its regulatory flexibility and lower costs, China has become a top destination for drugmakers like Bristol Myers looking to beef up their pipelines. Bristol Myers has struggled with looming patent expirations and clinical setbacks. But executives say the company is entering a data-rich period that will yield a younger and more diverse portfolio for the future. '

Drug ApprovalClinical ResultADCPatent Expiration

20 Feb 2026

·www.einpresswire.com

From early escape to immune evasion: Mapping drug resistance in advanced gastric cancer

GA, UNITED STATES, February 20, 2026 / EINPresswire.com / -- A next-generation antibody–drug conjugate has transformed treatment for HER2-positive gastric cancer , yet many patients fail to benefit or relapse rapidly. Using single-cell analysis of patient tumor samples, researchers uncovered distinct mechanisms that drive both early and late resistance to trastuzumab deruxtecan. The study shows that tumors resistant from the outset are marked by a mucus-associated protein that limits drug binding, while cancers that relapse later suppress drug activation and reshape their immune environment. By linking cellular heterogeneity, metabolic reprogramming, and immune escape, the findings reveal why a highly potent therapy can lose effectiveness—and point to biomarkers and combination strategies that could help restore durable responses. HER2-positive gastric cancer accounts for a substantial proportion of advanced cases and has long been treated with HER2-targeted therapies. While trastuzumab deruxtecan has shown superior activity compared with earlier agents, most patients either fail to respond initially or eventually develop resistance. Tumor heterogeneity, metabolic adaptation, and changes in the tumor microenvironment are believed to play critical roles, yet these processes remain poorly understood in clinical samples. Traditional bulk analyses obscure rare but influential cell populations that may drive resistance. In light of these challenges, a deeper investigation into treatment-induced cellular evolution and resistance mechanisms at single-cell resolution is urgently needed. Researchers from Peking University Cancer Hospital and collaborating institutions report new insights into drug resistance in advanced gastric cancer in a study published on 19 December 2025 in Precision Clinical Medicine. Analyzing tumor biopsies from patients enrolled in the phase II DESTINY-Gastric06 trial, the team applied single-cell RNA sequencing to track how cancer cells and their surrounding immune environment evolve during treatment with trastuzumab deruxtecan. The work identifies molecular drivers of both primary and acquired resistance and highlights potential biomarkers and therapeutic targets to improve patient outcomes. The researchers profiled nearly 92,000 individual cells from gastric cancer biopsies collected before treatment, during response, and after resistance emerged. By dissecting epithelial tumor cells at single-cell resolution, they identified distinct transcriptional programs linked to different resistance stages. Tumors showing primary resistance were enriched for metabolic pathways associated with glycolysis and lipid metabolism. Among these, MUC3A stood out as a key marker: high expression predicted shorter progression-free survival and experimentally reduced sensitivity to trastuzumab deruxtecan by limiting drug binding to HER2-positive cells. In contrast, acquired resistance followed a different trajectory. As treatment progressed, tumor cells downregulated HER2 and cell-cycle genes while upregulating CST3, a natural inhibitor of lysosomal proteases required to cleave the drug's linker and release its cytotoxic payload. Functional assays confirmed that CST3 dampens drug activation, allowing tumor cells to survive despite continued therapy. Beyond tumor-intrinsic changes, the study revealed dynamic remodeling of the tumor microenvironment. Initial treatment enhanced immune-cell infiltration and antigen presentation, but resistant tumors shifted toward an immunosuppressive state marked by reactivation of transforming growth factor-beta signaling and increased PD-1 expression on immune cells. Together, these findings show that resistance emerges through coordinated cellular, metabolic, and immune adaptations. "Resistance to highly effective therapies is rarely driven by a single factor," said one of the senior investigators. "By examining tumors at single-cell resolution, we were able to see how different cancer cell populations adapt in distinct ways—some blocking drug binding early on, others disabling drug activation or reshaping the immune environment over time. This layered view of resistance helps explain why responses can be short-lived and underscores the importance of dynamic biomarkers when treating advanced gastric cancer." The findings suggest several clinical strategies to improve outcomes for patients with HER2-positive gastric cancer. Measuring MUC3A expression could help identify patients unlikely to benefit from trastuzumab deruxtecan upfront, enabling more precise treatment selection. Targeting CST3 or restoring lysosomal drug processing may help overcome acquired resistance. In parallel, the observed shift toward immune suppression supports combining trastuzumab deruxtecan with immunotherapies or agents targeting TGF-β signaling. More broadly, the study demonstrates how single-cell technologies can guide personalized combination therapies by revealing when and how tumors adapt under therapeutic pressure. References DOI 10.1093/pcmedi/pbaf038 Original Source URL https://doi-org.libproxy1.nus.edu.sg/10.1093/pcmedi/pbaf038 Funding information Funding support for the study was provided by the Beijing Xisike Clinical Oncology Research Foundation (No. Y-2022HER2AZMS-0377 to Z.P.), Beijing Natural Science Foundation (grant number 7242088 to X.W.), and the National Natural Science Foundation of China (grant number 82473050 to X.W.). Lucy Wang BioDesign Research email us here Legal Disclaimer: EIN Presswire provides this news content "as is" without warranty of any kind. We do not accept any responsibility or liability for the accuracy, content, images, videos, licenses, completeness, legality, or reliability of the information contained in this article. If you have any complaints or copyright issues related to this article, kindly contact the author above.

Phase 2ImmunotherapyClinical Result

100 Deals associated with Fam-trastuzumab deruxtecan-NXKI

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External Link

KEGG	Wiki	ATC	Drug Bank
-	Fam-trastuzumab deruxtecan-NXKI	L01XC	DB14962

R&D Status

Approved

10 top approved records.

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Indication	Country/Location	Organization	Date
Stomach Cancer	India	AstraZeneca PLC	07 Oct 2025
HER2 Positive Solid Tumors	United Kingdom	Daiichi Sankyo UK Ltd.	09 Apr 2025
HR-positive/HER2-low Breast Carcinoma	United States	Daiichi Sankyo Co., Ltd.	28 Jan 2025
Hormone receptor positive HER2 positive breast cancer	South Korea	Daiichi Sankyo Co., Ltd.	19 Sep 2022
HER2 mutant non-small cell lung cancer	United States	Daiichi Sankyo, Inc.	11 Aug 2022
HER2 Positive Stomach Adenocarcinoma	Australia	AstraZeneca Pty Ltd.	08 Oct 2021
HER2-Low Breast Carcinoma	Australia	AstraZeneca Pty Ltd.	08 Oct 2021
Metastatic breast cancer	Canada	AstraZeneca Canada, Inc.	15 Apr 2021
HER2 positive Gastroesophageal Junction Adenocarcinoma	United States	Daiichi Sankyo, Inc.	15 Jan 2021
HER2-positive gastric cancer	Japan	Daiichi Sankyo Co., Ltd.	25 Sep 2020
HER2 Positive Breast Cancer	United States	Daiichi Sankyo, Inc.	20 Dec 2019

Developing

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Solid tumor	Phase 3	United States	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	China	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	Japan	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	Australia	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	Brazil	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	France	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	Israel	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	Italy	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	South Korea	Daiichi Sankyo, Inc.	23 Dec 2025
Solid tumor	Phase 3	Spain	Daiichi Sankyo, Inc.	23 Dec 2025

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Clinical Result

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Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT06731478 (DESTINY-Gastric05, ASCO_GI2026)	Phase 3	Metastatic HER2 positive gastroesophageal junction cancer First line HER2+	726	T-DXd + 5-FU (or CAPE) + pembrolizumab	plvftagyip(hjekknywmd) = mwqxpgrigc wlsjcpzhgn (tzdtedshlp )	Positive	08 Jan 2026
				Trastuzumab + platinum-based chemo + pembrolizumab	plvftagyip(hjekknywmd) = rcnauzxvsa wlsjcpzhgn (tzdtedshlp )
NCT04379596 (DESTINY-Gastric03 (DG-03), ASCO_GI2026)	Phase 1/2	Adenocarcinoma of Esophagus \| HER2-Low Gastric Cancer \| Gastroesophageal junction adenocarcinoma First line HER2-low	30	trastuzumab deruxtecan+volrustomig+fluoropyrimidine	erkjlinjqu(hfyqqbrsss) = mnkfimzsbn rgawqsdceg (jqnqvbkwry, 8.1 - NE)	Positive	08 Jan 2026
NCT06764875 (ARTEMIDE-Gastric01, ASCO_GI2026)	Phase 3	Metastatic HER2 positive gastroesophageal junction cancer First line HER2-positive \| PD-L1 CPS ≥1	840	rilvegostomig + T-DXd + investigator’s choice of capecitabine or 5-fluorouracil (5-FU)	qvgpcvtflm(pprrggisfq) = rhcoamrvaf zhwdhyfqnj (pftrmqdixh, 24.9 - NR)	Positive	08 Jan 2026
				rilvegostomig + trastuzumab + investigator’s choice of FP or CAPOX	udvdhctdyv(rvpmfzeefd) = iiflcfuibz ttrehjsvqk (cgcdetzqog, 17.0 - NR) View more
ASCO_GI2026	Not Applicable	HER2-positive gastric cancer \| HER2 positive Gastroesophageal Junction Adenocarcinoma HER2-positive	915	Trastuzumab deruxtecan	euzarcgjgh(rhdjtthuba) = iernlyibwa uzgiqrlaaa (ztgscmvelk ) View more	Positive	08 Jan 2026
NCT03529110 (DESTINY-Breast03, SABCS2025) Manual	Phase 3	Metastatic human epidermal growth factor 2 positive carcinoma of breast HER2 Positive	524	Trastuzumab deruxtecan (T-DXd) 5.4 mg/kg	gxtddcgojy(fdxxbmdfwi) = kzoafadrsr ijfpcyhpgh (ewdqdgylol, 49.4 - 67.0) View more	Positive	12 Dec 2025
				Trastuzumab emtansine (T-DM1) 3.6 mg/kg	gxtddcgojy(fdxxbmdfwi) = sjuidrtpmr ijfpcyhpgh (ewdqdgylol, 35.4 - 52.6) View more
SABCS2025	Not Applicable	HER2-Low Breast Carcinoma HER2-low	126	Trastuzumab deruxtecan	zibgfflris(dxbbsrwmux) = swzchxbbjc cbatpsxvwf (rtrugceuom )	Positive	12 Dec 2025
				Trastuzumab deruxtecan (HR positive and PR expression ≤ 10%)	zibgfflris(dxbbsrwmux) = uvqjnzcmmf cbatpsxvwf (rtrugceuom )
SABCS2025	Not Applicable	Metastatic human epidermal growth factor 2 positive carcinoma of breast HER2-positive	540	5HT3 receptor antagonist + dexamethasone	jnegexveqw(ebyibwjptn) = hgwgpstdgf fdqlzzxzjo (thaooqcsnh ) View more	Positive	12 Dec 2025
				NK1 receptor antagonist + 5HT3 receptor antagonist + dexamethasone	jnegexveqw(ebyibwjptn) = plpgypmnpp fdqlzzxzjo (thaooqcsnh ) View more
SABCS2025	Not Applicable	HER2 Positive Breast Cancer \| Brain metastases Second line HER2+	255	trastuzumab deruxtecan	whfpoezqfk(vtwweseyjc) = wixmajuoxg nrflcycdgq (gkcckkhoth )	Positive	12 Dec 2025
				tucatinib+trastuzumab+capecitabine	whfpoezqfk(vtwweseyjc) = oquplorzsc nrflcycdgq (gkcckkhoth )
NCT03523585 (DESTINY-Breast12, SABCS2025)	Phase 2/3	Metastatic human epidermal growth factor 2 positive carcinoma of breast Second line HR-positive \| HER2+	262	Trastuzumab deruxtecan (HR+)	sqonxwdsnw(trwsjhrqxb) = neutropenia (12.1%), anemia (7.3%), and fatigue (6.7%) in the HR+ subgroup, and neutropenia (11.3%), decreased neutrophil count (8.2%), and anemia (7.2%) in the HR− subgroup. hmezpjohim (oexcstiawl )	Positive	12 Dec 2025
				Trastuzumab deruxtecan (HR−)
NCT04538742 (DESTINY-Breast07, SABCS2025)	Phase 1/2	HER2 Positive Breast Cancer First line HER2+	125	Trastuzumab deruxtecan (T-DXd)	ajozstxwjh(trotogweim) = onpqyukrhv hxmpaoocky (iewfauugjc ) View more	Positive	12 Dec 2025
				T-DXd + pertuzumab	ajozstxwjh(trotogweim) = tcpmoihoni hxmpaoocky (iewfauugjc ) View more

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Fam-trastuzumab deruxtecan-NXKI

Overview

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