{"id":2531,"date":"2025-11-04T15:31:26","date_gmt":"2025-11-04T15:31:26","guid":{"rendered":"https://www.lunit.io/en/?post_type=publication&#038;p=2531"},"modified":"2025-11-17T15:35:17","modified_gmt":"2025-11-17T15:35:17","slug":"phase-1-study-of-imc-002-a-next-generation-anti-cd47-antibody-in-advanced-solid-tumors","status":"publish","type":"publication","link":"https://lunit.supremeclients.com/ko/publication/phase-1-study-of-imc-002-a-next-generation-anti-cd47-antibody-in-advanced-solid-tumors/","title":{"rendered":"Phase 1 Study of IMC-002, a Next-Generation Anti-CD47 Antibody, in Advanced Solid Tumors"},"content":{"rendered":"<div class=\"col-span-12 mt-2 bg-white md:mt-0\">\n<div class=\"hero-title\">\n<h3>Phase 1 Study of IMC-002, a Next-Generation Anti-CD47 Antibody, in Advanced Solid Tumors</h3>\n</div>\n</div>\n<div class=\"bg-white\">\n<div id=\"xref-fn-1-1\" class=\"relative mb-[20px]\" data-testid=\"author-affiliations-list\"></div>\n</div>\n<p>Jin Seok Ahn, Jung Yong Hong, Joon Oh Park, Sung Young Lee, SuYeon Kim, Hwi-yeol Yun, Chan-Young Ock, Woochan Hwang, Sung Ho Kim, Heung Tae Kim, Ho Yeong Lim</p>\n<p><strong>Cancer Research and Treatment, 2025</strong></p>\n<p><strong>Abstract</strong></p>\n<div class=\"abstract-section\">\n<div id=\"abspara0010\" role=\"paragraph\"><b>Purpose</b><br>\nIMC-002 is a fully human cluster of differentiation 47-targeted immunoglobulin G4 monoclonal antibody, designed to minimize off-target effects. This study (NCT05276310) assessed its safety/tolerability and preliminary anti-tumor activity in patients with advanced solid tumors who were not eligible for or had progressed on standard treatment.<br>\n<b>Materials and Methods</b><br>\nHere we report results from the initial 3 + 3 design dose-escalation part of a two-part Phase 1, open-label, dose-escalation/expansion study. IMC-002 was administered intravenously every 2 weeks at four doses (5, 10, 20, and 30 mg/kg). The primary objective was to assess safety/tolerability, including maximum tolerated dose (MTD) and recommended Phase 2 dose (RP2D). Secondary objectives included pharmacokinetics and clinical activity, including best overall response (BOR), disease control rate (DCR), and clinical benefit rate (CBR).<br>\n<b>Results</b><br>\nTwelve patients were included in total, with three per dose level. Most patients (11/12) had stage IV disease; 7/12 had received three prior systemic therapies. No dose-limiting toxicities were observed and MTD was not reached. The most common treatment-related adverse events (TRAEs) were rash (9/12), vitreous floaters (8/12), and (hemolytic) anemia (5/12). There was no treatment-related thrombocytopenia, neutropenia, or infection. IMC-002 had dose-proportional pharmacokinetics, achieving steady state levels from Cycle 2. BOR was stable disease in six patients (DCR 50.0%). CBR was 33% (four patients maintaining disease control for ≥6 months).<br>\n<b>Conclusion</b><br>\nIMC-002 demonstrated favorable safety/tolerability at doses of 5–30 mg/kg every 2 weeks. RP2D was defined as 20 mg/kg every 3 weeks. Preliminary anti-tumor activity was observed, with a CBR of 33%.</div>\n</div>\n<p style=\"text-align: center;\"><a href=\"https://www.e-crt.org/journal/view.php?number=3859\"><b>Read the full paper</b></a></p>\n","protected":false},"featured_media":0,"template":"","publication-oncology":[86,94],"publication-region":[87],"publication-type":[],"radiology":[],"class_list":["post-2531","publication","type-publication","status-publish","hentry","publication-oncology-others","publication-oncology-peer-reviewed-clinical-papers","publication-region-asia"],"acf":[],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.6 - https://yoast.com/product/yoast-seo-wordpress/ -->\n<title>Phase 1 Study of IMC-002, a Next-Generation Anti-CD47 Antibody, in Advanced Solid Tumors - Lunit</title>\n<meta name=\"robots\" content=\"index, follow, max-snippet:-1, max-image-preview:large, max-video-preview:-1\">\n<link rel=\"canonical\" href=\"https://fr.lunit.supremeclients.com/publication/phase-1-study-of-imc-002-a-next-generation-anti-cd47-antibody-in-advanced-solid-tumors/\">\n<meta property=\"og:locale\" content=\"ko_KR\">\n<meta property=\"og:type\" content=\"article\">\n<meta property=\"og:title\" content=\"Phase 1 Study of IMC-002, a Next-Generation Anti-CD47 Antibody, in Advanced Solid Tumors - Lunit\">\n<meta property=\"og:description\" content=\"Phase 1 Study of IMC-002, a Next-Generation Anti-CD47 Antibody, in Advanced Solid Tumors Jin Seok Ahn, Jung Yong Hong, Joon Oh Park, Sung Young Lee, SuYeon Kim, Hwi-yeol Yun, Chan-Young Ock, Woochan Hwang, Sung Ho Kim, Heung Tae Kim, Ho Yeong Lim Cancer Research and Treatment, 2025 Abstract Purpose IMC-002 is a fully human cluster […]\">\n<meta property=\"og:url\" content=\"https://fr.lunit.supremeclients.com/publication/phase-1-study-of-imc-002-a-next-generation-anti-cd47-antibody-in-advanced-solid-tumors/\">\n<meta property=\"og:site_name\" content=\"Lunit\">\n<meta property=\"article:modified_time\" content=\"2025-11-17T15:35:17+00:00\">\n<meta name=\"twitter:card\" content=\"summary_large_image\">\n<meta name=\"twitter:site\" content=\"@lunit_ai\">\n<meta name=\"twitter:label1\" content=\"예상 되는 판독 시간\">\n\t<meta name=\"twitter:data1\" content=\"2분\">\n<script type=\"application/ld+json\" class=\"yoast-schema-graph\">{\"@context\":\"https://schema.org\",\"@graph\":[{\"@type\":\"WebPage\",\"@id\":\"https://fr.lunit.supremeclients.com/publication/phase-1-study-of-imc-002-a-next-generation-anti-cd47-antibody-in-advanced-solid-tumors/\",\"url\":\"https://fr.lunit.supremeclients.com/publication/phase-1-study-of-imc-002-a-next-generation-anti-cd47-antibody-in-advanced-solid-tumors/\",\"name\":\"Phase 1 Study of IMC-002, a Next-Generation Anti-CD47 Antibody, in Advanced Solid Tumors - 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