echemi logo
Product
  • Product
  • Supplier
  • Inquiry
    Home > Medical News > Latest Medical News > Can more than 10 Chinese companies develop CLDN 18.2 as the "black horse" of immunotherapy?

    Can more than 10 Chinese companies develop CLDN 18.2 as the "black horse" of immunotherapy?

    • Last Update: 2020-07-30
    • Source: Internet
    • Author: User
    Search more information of high quality chemicals, good prices and reliable suppliers, visit www.echemi.com
    CLDN 18.2 is a tightly connected protein molecule that has been seen by researchers as a potential target for developing solid tumor immunotherapy such as stomach cancer.no treatments for CLDN 18.2 have been approved worldwide., companies such as Astellas and Amin are developing CLDN 18.2 targeted therapy., according to incomplete statistics, in China, including Cozi Bio, Chongsheng Group, Osaikang Pharmaceuticals, including more than 10 companies have also laid out this area., what is the development potential of CLDN 18.2? Why is it so popular with pharmaceutical companies? The biological role of the Claudin protein Claudins protein is a tightly connected (tight junction) molecule.close connection, also known as the locked band, is common in vertebrates of various epithelial and endothelial cells, in the gastrointestinal cortex between the connection stakes are particularly common.structurally, the tight connection consists of rows of protein particles, which form a continuous fiber that closes the gap between adjacent cells, allowing only water molecules and ions to pass through small holes at the junction, making it difficult for macromolecules to pass through.close connections have been shown to be the main determinant of cell bypass.plays an important role in human life activities.on the one hand, close connection can exercise the function of "barrier", the size and charge of the substance to choose, and then regulate the cell side of the way of the material transport.for example, cerebrovascular endothelial cells can pass through this barrier to prevent blood from mixing with brain extracellular fluid, and so on.on the other hand, close connection swells the function of "fence" and maintains the polarity of the cell by regulating the free dispersion of lipids and proteins between the two functional areas of the top and substrate side membranes.the structure of the Claudin protein (Photo: References) Structurally, the tight connection is a complex composed of a variety of proteins, such as transmembrane proteins and cytoplasm, and its stability requires the coordinated activity of several different proteins, of which Claudin protein plays a major role.Claudin protein was first discovered in 1998 and is a four-time transmembrane protein with a molecular weight of about 20 to 27 kDa, with the C and N ends convextous to the cytoplasm side, as well as two extracellular domains, ECL1 and ECL2.studies have found that the closely connected Claudin protein is present in its subtype, and the closely connected permeability is regulated by the interaction between different Claudin protein subtypes.Claudin 18.2 and cancer Claudins protein are mainly expressed in epithelial cells, and its function is mainly to regulate the permeability of the barrier structure.studies have shown that changes in the expression of Claudin protein can lead to impaired close connection function, affect signaling pathways, and play a tumor-promoting role in some epithelial cancers.Claudin protein has been found to be abnormally expressed in a variety of cancers, including stomach cancer, hepatocellular carcinoma, biliary cancer, breast cancer, kidney cell carcinoma, pancreatic cancer, non-small cell lung cancer and mesothelioma.has so far identified at least 27 members of the Claudin protein family, of which CLDN 18 has two isomers, CLDN 18.1 and CLDN 18.2.studies have shown that the expression of CLDN 18.2 protein is tissue-specific and is expressed mainly in stomach and stomach adenocarcinoma tissue.in normal physiological conditions, CLDN 18.2 is expressed only in the differentiated epithelial cells on the gastric mucosa, but not in other healthy tissues.However, in many types of primary and post-metastatic cancers, CLDN 18.2 protein molecules have also been found to be expressed in large quantities, such as CLDN 18.2 proteinin in 50%-80% of stomach cancer patients., in addition, in pancreatic cancer, esophageal cancer, ovarian cancer and other tumors, CLDN 18.2 also exists the phenomenon of active expression.highly specific expression in normal tissues, combined with active expression in a variety of cancers, makes the CLDN 18.2 protein an ideal target for researchers to develop solid tumor immunotherapy such as gastric and pancreatic cancers.no global approval siseine has been approved, and at least a dozen Chinese companies are developing CLDN18.2 as a potential target for the development of solid tumor-targeted therapies, but research in this area has been relatively muted.it wasn't until 2016, when Ganymed announced the results of a clinical trial of its CLDN 18.2-embedded antibody zolbetuximab at the ASCO conference that CLDN 18.2, an anti-cancer molecular target, attracted wider industry attention, and Astellas immediately acquired Ganymed that year., according to incomplete statistics, in China, at least a dozen companies are developing innovative treatments that target CLDN 18.2, not only monotophosis, but also bi-resistance and CAR-T therapy.the following excerpts are shared with readers of research-in-the-drug information developed globally and in China.1, zolbetuximab (IMAB362) Drug Action Mechanism: CLDN 18.2 Antibody Company: Astellas IMAB362 is an antibody developed by Ganymed to target the CLDN 18.2 protein.at the ASCO meeting in June 2016, Ganymed published data from a phase 2 clinical trial of zolbetuximab for gastric cancer patients, showing that zolbetuximab and chemotherapy increased the median total survival of patients from 8.4 months to 13.2 months;the release of this stunning data made zolbetuximab the "black horse" at the ASCO meeting that year, and the CLDN 18.2 target has since attracted wider attention in the industry.October 2016, Astellas successfully took down zolbetuximab's revenue by acquiring Ganymed for $1.4 billion.ClinicalTrial.gov website, Zolbetuximab is currently conducting several clinical trials in tumors such as gastric cancer, gastric esophagus combination adenocarcinoma and pancreatic cancer. include a Phase 3 clinical trial designed to assess the efficacy of zolbetuximab in combination with mFOLFOX6 first-line treatment CLDN 18.2 positive, HER2-negative local progression non-removable or metastatic gastric or gastroesophageal adenocarcinoma. in China, Astellas has submitted a clinical application for zolbetuximab in November 2018 and has been approved for clinical trials for adaptation for a combination of platinum and fluorourea-based chemotherapy for locally advanced non-removability or metastasis, CLDN 18.2 positive and FIRST-line treatment of patients with HER2-negative adult gastric and gastroesophageal cancer. 2, AMG910 Drug Action Mechanism: CD3/CLDN 18.2 Bispecific Antibodies Company: Amjin, BaijiShenzhou AMG910 is a targeted CD3 and CLDN 18.2 dual antibody drugs developed by Amjin. worldwide, Amgen is conducting a Phase 1 clinical study to assess the safety, tolerance, pharmacokinetics and efficacy of Patients with CLDN 18.2-positive gastric and gastroesophageal adenocarcinoma patients with AMG 910. in China, Amin and Baiji Shenzhou have jointly submitted a clinical trial application for AMG910, which was accepted by CDE on July 1 this year. 3, CT041, AB011 Drug Action Mechanism: TARGETING CLDN18.2 CAR-T Therapy, CLDN18.2 Single Resistance Company: Cozi Bio CT041 is a human-derived co-development of Kozi Bio Anti-CLDN 18.2 self-car T cell injection, to be developed to treat CLDN18.2 positive, past systematic treatment after progress or recurrence of advanced gastric adenocarcinoma / esophageal gastric binding adenocarcinoma, pancreatic cancer and other indications. the clinical effectofs of CAR-T therapy have been proven in blood cancer, but the application bottleneck in solid tumors has yet to be broken, so CT041 is expected to bring new options for patients with solid tumors. Based on the car-T clinical data released earlier by Cozibios in the treatment of gastric/pancreatic cancer: of the 12 patients treated, 8 experienced varying degrees of tumor decline, especially in an improved treatment subgroup, 5 of them achieved objective remission (one of which was confirmed for objective remission) and one achieved full remission. in May this year, the drug was approved for clinical use in the United States, cozibiosis said in a press release, which is the first international trial license for CLDN 18.2 CAR-T cell candidate drug. AB011 is a recombinant humanized anti-CLDN 18.2 monoclonal antibody injection developed by Cozibio, which was approved in Clinical Trials in China in December last year and is intended to be developed to treat patients with CLDN 18.2-positive solid tumors. 4, TST001 Drug Action Mechanism: CLDN18.2 Monoantine Company: Syngdald Group TST001 is a subsidiary of The sun-to-sheng Group, Mybos Bio independent research and development of CLDN 18.2 humanized monoclonal antibody new drugs, through High affinity-specific combination of CLDN 18.2 proteins, mediated antibody-dependent cytotoxicity (ADCC) and complement-dependent cytotoxicity (CDC) mechanisms, directly targeting the killing of CLDN 18.2-expressed tumor cells. with advanced process technology, TST001's rock algal sugar modification ratio can be greatly reduced in production, further enhancing TST001's tumor killing activity. in April this year, TST001 has been approved in China and the United States for clinical trials. in China, TST001 has been approved for clinical studies of single-drug or combined standard therapy for the treatment of CLDN18.2-positive advanced solid tumors, including, but not limited to, gastric/gastroesophageal combination adenocarcinoma, pancreatic catheter adenocarcinoma, bile duct cancer, etc. On July 1, , Transingroup announced that TST001 had successfully completed the first patient administration in Phase 1 clinical study conducted in the United States, the main purpose of which was to assess the safety, tolerance and recommended dose of TST001 in subjects with advanced or metastatic solid tumors. 5, ASKB589 Injection Drug Action Mechanism: CLDN18.2 Antibody Company: Oseikang Pharmaceuticals ASKB589 Injection is an independent research and development of Oseikang, with independent intellectual property rights of a human-derived CLDN 18.2 antibody, the drug in the research mainly through antibody-dependent cell toxicity (ACCD) and supplement-dependent cell toxicity (CDC) anti-tumor tumor, to be used in gastric and gastrointestinal combination cancer. April this year, the drug has been approved for clinical treatment in China, clDN 18.2 positive local late or metastatic gastric and gastric esophagus binding adenocarcinoma, pancreatic cancer and other malignant solid tumors. 6, SPX-301, SPX-101 Drug Action Mechanism: CLDN 18.2/PD-L1 Double Resistance, CLDN 18.2 Single Resistance Company: Sparx Therapeutics SPX-301 Yes Sparx developed a dual-specific antibody drug targeting both CLDN 18.2 and PD-L1, built using Sparx's SMARTOPTM model with independent intellectual property rights, and segmented optimization using its LEMMAbTM phage display technology. it is understood that this is by far the world's first CLDN 18.2/PD-L1 double specific antibody. at the AACR meeting in June, Sparx released preclinical research data on the drug. animal experiments showed that SPX-301 had similar pharmacodynamic characteristics to monoclonal antibodies, and the level of anti-drug antibodies (ADA) in mice was very low, so it was possible that immunogenicity and safety were good. mice inoculation experiments showed that SPX-301 can effectively inhibit the growth of MC38 tumors with stable expression OF CLDN 18.2. SPX-101 is a CLDN 18.2 monogenita developed by Sparx. preclinical studies showed that SPX-101 had a high affinity for CLDN 18.2, and SPX-101 was positively correlated with the intake of 803 cells of stomach cancer and the expression level of CLDN18.2. In addition, the drug dynamics characteristics of PX-101 in mice and rats were also ideal, not only with a longer half-life and a lower level of anti-drug antibodies. mouse vaccination models showed that SPX-101 performed well in tumor suppression in at least two tumor models. it is worth mentioning that in November 2018, Kun Pharmaceutical Group has signed an agreement with Sparx to develop a new class of CLDN 18.2 humanized monoclonal antibodies for the treatment of stomach cancer. , Sparx will be responsible for cell construction, screening, candidate antibody preparation and validation. In addition to the above-mentioned companies, there are a number of Chinese pharmaceutical companies in the development of CLDN 18.2 antibody drugs, including Tianguangshi Bio, Jikai Gene, Jianxin Biopharmaceuticals, Sanhe Pharmaceuticals, Van Nsen Bio, Ruiyang Pharmaceuticals, etc., these CLDN 18.2 antibodies in the majority of drugs are still in the preclinical research stage. summary No targeted CLDN18.2 therapy has been approved worldwide. currently developed by pharmaceutical companies to target this target in the form of research therapy is also relatively diverse, not only monotophos, but also bispecific antibodies and CAR-T therapy. from the perspective of indications, the existing clinical research mainly focuses on gastric and gastroesophageal combination adenocarcinoma, pancreatic cancer and other cancer species. <
    This article is an English version of an article which is originally in the Chinese language on echemi.com and is provided for information purposes only. This website makes no representation or warranty of any kind, either expressed or implied, as to the accuracy, completeness ownership or reliability of the article or any translations thereof. If you have any concerns or complaints relating to the article, please send an email, providing a detailed description of the concern or complaint, to service@echemi.com. A staff member will contact you within 5 working days. Once verified, infringing content will be removed immediately.

    Related Articles

    Contact Us

    The source of this page with content of products and services is from Internet, which doesn't represent ECHEMI's opinion. If you have any queries, please write to service@echemi.com. It will be replied within 5 days.

    Moreover, if you find any instances of plagiarism from the page, please send email to service@echemi.com with relevant evidence.