(Tc-99m-annexin V-128) - 药物靶点：Phosphatidylserine_在研适应症：强直性脊柱炎，肥大型心肌病，颈动脉狭窄_专利_临床

概要

基本信息

药物类型

重组蛋白、诊断用放射药物

别名

99mTc-rhAnnexin V-128、99mTechnetium-labelled rhAnnexin V-128、Tc-99m-recombinant human annexin V-128

+ [2]

靶点

Phosphatidylserine

作用机制

Phosphatidylserine抑制剂(磷脂酰丝氨酸抑制剂)、SPECT(单光子发射计算机断层成像术增强剂)

治疗领域

免疫系统疾病感染神经系统疾病+ [2]

在研适应症

强直性脊柱炎肥大型心肌病颈动脉狭窄+ [1]

非在研适应症

细菌性心内膜炎肿瘤血栓形成

原研机构

Advanced Accelerator Applications USA, Inc.

在研机构

AAA Pharmaceutical, Inc.

Advanced Accelerator Applications SA

Atreus GmbH

+ [1]

非在研机构

Advanced Accelerator Applications (UK & Ireland) Ltd.

最高研发阶段临床2期

首次获批日期-

最高研发阶段(中国)-

特殊审评-

序列信息

Sequence Code 315644294

关联

4

项与 Tc-99m-annexin V-128 相关的临床试验

NCT03232580 / Terminated临床2期

Phase II Study of 99mTc-rhAnnexin V-128 Radionuclide Imaging in Patients With Clinical Suspicion or Confirmed Diagnosis of Spondyloarthritis (SpA)

This single center, open-label, proof of concept (PoC) Phase II study aimed to assess the investigational imaging agent 99mTc-rhAnnexin V-128 in detecting spondyloarthritis (SpA) lesions.
Overall, it was planned to recruit 20 adults with suspected or confirmed SpA. First, 5 patients were enrolled into a "proof of concept" phase, to assess the imaging potential of 99mTc-rhAnnexin V-128 in terms of imaging quality, disease-lesion radiotracer uptake and medical relevance. Based on these results the Data Monitoring Committee (DMC) was to decide whether to terminate the study or whether to continue and enroll the next 15 planned patients.

开始日期2017-09-18

申办/合作机构

Advanced Accelerator Applications SA

NCT02459613 / Terminated临床1/2期

Evaluation de la rhAnnexine V-128 radiomarquée Dans le Diagnostic de l'Endocardite Infectieuse, du Thrombus Atrial et de Leurs Complications Emboliques associées

Intraluminal thrombi adherent to cardiac valves or atria share a common pathophysiology involving the aggregation of activated platelets with phosphatidylserine (PS) expression on the outer layer of the thrombus. They also share common complications, i.e. damages to the underlying myocardium and embolic risk related to thrombus fragmentation. The diagnostic work-up, currently relying on morphologic imaging alone (mainly echography), lacks sensitivity and does not allow to differentiate between active (renewal and growth activity) and quiescent (scarred) thrombus. It is therefore highly desirable to develop a new approach able to non-invasively provide insight on the biological activity of thrombi and to detect embolic events in a single exam.
Annexin V is a 36 kDa endogenous glycoprotein which binds PS with nanomolar affinity. Radiolabeled Annexin V has been shown to provide molecular imaging of PS expressed by apoptotic cells or activated platelets. The ability of the imaging agent to bind mural thrombus has been established in vivo in a murine model of abdominal aortic aneurysm and ex vivo in human. It has been also shown that radiolabeled Annexin V allowed in vivo detection of vegetations and secondary pulmonary emboli with high sensitivity in various animal models of infective endocarditis.
A radiolabeling kit of annexin V complying with GMP requirements has been developed (rhAnnexine V-128, Advanced Accelerator Applications - Atreus) and is currently available. AnniE is a single centre, proof of concept, interventional, open, non-randomized study aiming at evaluating the sensitivity of 99mTc-Annexin V-128 in the detection thrombus in comparison with reference imaging in patients presenting with either: 1/ infective endocarditis or 2/ atrial thrombus. The safety of the 99mTc-Annexin V-128 will be assessed in a first phase (10 first patients enrolled). Data in relation with safety of the imaging agent will be reviewed by an independent Data and Safety Monitoring Board (DSMB); in case of positive answer, the study will continue with a second phase. The data gathered in all patients (n=120) will be used to determine outcome measures.

开始日期2016-02-05

申办/合作机构

Institut National de la Santé et de la Recherche Médicale

[+1]

NCT02328027 / Terminated临床1/2期

A Phase I-IIa Study of Safety, Tolerance, Pharmacokinetics, Dosimetry and Benefice of Early Nuclear Medicine Imaging of 99mTc-rhAnnexin V-128 in Patients With Rheumatoid Arthritis or Ankylosing Spondylitis

This was a monocentric, open label, Phase I-IIa study. Eligible patients who signed the ICF received two single intravenous (IV) bolus of the imaging agent 99mTc-rhAnnexin V-128. The first dose was administered on Day 1, and the second dose on Day 42 (±2 weeks).
All patients were to start a new disease modifying treatment for RA or AS on Day 2. This disease modifying treatment was at the discretion of the investigator and was not chosen by the sponsor.
Safety was monitored at every visit. Whole body scintigraphic imaging was performed at Day 1 and Day 42 after 99mTc-rhAnnexin V-128 dosing. Clinical disease assessments were performed at screening, Day 42 and Day 90 to assess response to RA or AS treatment. Blood was drawn to test for 99mTc-rhAnnexin V-128 immunogenicity at screening and on Days 30, 56 and 90. Patients participating in the pharmacokinetic (PK)/dosimetric sub-study had additional assessments in the 24 hours following the Day 1 dose of 99mTc-rhAnnexin V-128.

开始日期2014-12-11

申办/合作机构

Advanced Accelerator Applications SA

100 项与 Tc-99m-annexin V-128 相关的临床结果

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100 项与 Tc-99m-annexin V-128 相关的转化医学

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100 项与 Tc-99m-annexin V-128 相关的专利（医药）

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30

项与 Tc-99m-annexin V-128 相关的文献（医药）

2020-10-01·Journal of the American College of Cardiology1区 · 医学

Molecular Imaging of Apoptosis in Atherosclerosis by Targeting Cell Membrane Phospholipid Asymmetry

1区 · 医学

Article

作者: Fuster, Valentin ; Mattis, Jeffrey A ; Nakahara, Takehiro ; Chaudhry, Farhan ; Petrov, Artiom ; Kim, Dongbin ; Ozaki, Yukio ; Arbustini, Eloisa ; Strauss, H William ; Chaudhry, Fayzan ; Narula, Jagat ; Kawai, Hideki ; Pak, Koon Y ; Adapoe, Matthew K M Y ; Shekhar, Aditya ; Narula, Navneet ; Blankenberg, Francis G ; Johnson, Kipp W ; Levy, Phillip D ; Tanimoto, Takashi

BACKGROUND:

Apoptosis in atherosclerotic lesions contributes to plaque vulnerability by lipid core enlargement and fibrous cap attenuation. Apoptosis is associated with exteriorization of phosphatidylserine (PS) and phosphatidylethanolamine (PE) on the cell membrane. Although PS-avid radiolabeled annexin-V has been employed for molecular imaging of high-risk plaques, PE-targeted imaging in atherosclerosis has not been studied.

OBJECTIVES:

This study sought to evaluate the feasibility of molecular imaging with PE-avid radiolabeled duramycin in experimental atherosclerotic lesions in a rabbit model and compare duramycin targeting with radiolabeled annexin-V.

METHODS:

Of the 27 rabbits, 21 were fed high-cholesterol, high-fat diet for 16 weeks. Nine of the 21 rabbits received ^99mTc-duramycin (test group), 6 received ^99mTc-linear duramycin (duramycin without PE-binding capability, negative radiotracer control group), and 6 received ^99mTc-annexin-V for radionuclide imaging. The remaining normal chow-fed 6 animals (disease control group) received ^99mTc-duramycin. In vivo microSPECT/microCT imaging was performed, and the aortas were explanted for ex vivo imaging and for histological characterization of atherosclerosis.

RESULTS:

A significantly higher duramycin uptake was observed in the test group compared with that of disease control and negative radiotracer control animals; duramycin uptake was also significantly higher than the annexin-V uptake. Quantitative duramycin uptake, represented as the square root of percent injected dose per cm (√ID/cm) of abdominal aorta was >2-fold higher in atherosclerotic lesions in test group (0.08 ± 0.01%) than in comparable regions of disease control animals (0.039 ± 0.0061%, p = 3.70·10^-8). Mean annexin uptake (0.060 ± 0.010%) was significantly lower than duramycin (p = 0.001). Duramycin uptake corresponded to the lesion severity and macrophage burden. The radiation burden to the kidneys was substantially lower with duramycin (0.49% ID/g) than annexin (5.48% ID/g; p = 4.00·10^-4).

CONCLUSIONS:

Radiolabeled duramycin localizes in lipid-rich areas with high concentration of apoptotic macrophages in the experimental atherosclerosis model. Duramycin uptake in atherosclerotic lesions was significantly greater than annexin-V uptake and produced significantly lower radiation burden to nontarget organs.

2018-12-01·Arthritis research & therapy2区 · 医学

Evaluation of 99mTc-rhAnnexin V-128 SPECT/CT as a diagnostic tool for early stages of interstitial lung disease associated with systemic sclerosis

2区 · 医学

ArticleOA

作者: Schibli, Roger ; Maurer, Britta ; Guo, Li ; Béhé, Martin ; Distler, Oliver ; Brunner, Matthias ; Schniering, Janine ; Ye, Shuang

BACKGROUND:

Given the need for early detection of organ involvement in systemic sclerosis, we evaluated ^99mTc-rhAnnexin V-128 for the detection of early stages of interstitial lung disease (ILD) in respective animal models using single photon emission computed tomography (SPECT/CT).

METHODS:

In bleomycin (BLM)-challenged mice, fos-related antigen 2 (Fra-2) transgenic (tg) mice and respective controls, lung injury was evaluated by analysis of hematoxylin and eosin (HE) and Sirius red staining, with semi-quantification of fibrosis by the Ashcroft score. Apoptotic cells were identified by TUNEL assay, cleaved caspase 3 staining and double staining with specific cell markers. To detect early stages of lung remodeling by visualization of apoptosis, mice were injected intravenously with ^99mTc-rhAnnexin V-128 and imaged by small animal SPECT/CT. For confirmation, biodistribution and ex vivo autoradiography studies were performed.

RESULTS:

In BLM-induced lung fibrosis, inflammatory infiltrates occurred as early as day 3 with peak at day 7, whereas pulmonary fibrosis developed from day 7 and was most pronounced at day 21. In accordance, the number of apoptotic cells was highest at day 3 compared with saline controls and then decreased over time. Epithelial cells (E-cadherin+) and inflammatory cells (CD45+) were the primary cells undergoing apoptosis in the earliest remodeling stages of experimental ILD. This was also true in the pathophysiologically different Fra-2 tg mice, where apoptosis of CD45+ cells occurred in the inflammatory stage. In accordance with the findings on tissue level, at day 3 in the BLM and at week 16 in the Fra-2 tg model, biodistribution and/or ex vivo autoradiography showed increased pulmonary uptake of ^99mTc-rhAnnexin V-128 compared with controls. However, accumulation of the radiotracer and thus the signal intensity in lungs was too low to allow the differentiation of healthy and injured lungs in vivo.

CONCLUSION:

At the tissue level, ^99mTc-rhAnnexin V-128 successfully demonstrated early stages of ILD in two animal models by detection of apoptotic epithelial and/or inflammatory cells. In vivo, however, we did not detect early lung injury. It remains to be investigated whether the same applies to human ILD.

2018-08-01·Journal of nuclear cardiology : official publication of the American Society of Nuclear Cardiology

Correction to: Radiopharmaceutical tracers for cardiac imaging

作者: Nishii, Ryuichi ; Zhang, Ming-Rong ; Kikuchi, Tatsuya ; Manabe, Osamu ; Suzuki, Eriko ; Yoshinaga, Keiichiro ; Scholte, Arthur J H A ; El Mahdiui, Mohammed

Regrettably the original version of the above article contained errors in the three chemical structures presented in the 'Atherosclerosis imaging' section of Table 5, namely: ^99mTc annexin V, ⁶⁸Ga DOTATATE, and ⁶⁴Cu DOTATATE; the chemical structures have been corrected in Table presented here. In addition, the radiopharmaceutical for isotope ⁶⁷Ga has been corrected to ⁶⁷Ga citrate, and many of the radiopharmaceuticals presented at the end of the table have been corrected.

100 项与 Tc-99m-annexin V-128 相关的药物交易

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研发状态

10 条进展最快的记录,

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适应症	最高研发状态	国家/地区	公司	日期
脊椎关节炎	临床2期	美国	Advanced Accelerator Applications SA	2017-09-18
细菌性心内膜炎	临床2期	法国	Advanced Accelerator Applications SA	2016-02-05
血栓形成	临床2期	法国	Advanced Accelerator Applications SA	2016-02-05
强直性脊柱炎	临床2期	瑞士	Advanced Accelerator Applications SA	2014-12-11
类风湿关节炎	临床2期	瑞士	Advanced Accelerator Applications SA	2014-12-11
心肌疾病	临床2期	加拿大	Advanced Accelerator Applications (UK & Ireland) Ltd.	-
肥大型心肌病	临床2期	-	AAA Pharmaceutical, Inc.	-
肥大型心肌病	临床2期	-	Advanced Accelerator Applications SA	-
肥大型心肌病	临床2期	-	Atreus GmbH	-
肥大型心肌病	临床2期	-	Atos SE	-

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临床结果

适应症

分期

评价

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT02328027 (CTgov)	临床1/2期	类风湿关节炎 \| 强直性脊柱炎	16	99mTc-rhAnnexin V-128 (99mTc-rhAnnexin V-128: Ankylosing Spondylitis)	壓齋壓簾構鑰獵醖艱繭(廠壓餘積鹹艱鹽鬱範夢) = 齋鏇廠鏇鹽衊顧壓鑰鏇壓繭艱廠範淵醖鏇構壓 (廠夢網築膚鹽夢顧膚夢, 鹽膚積襯艱積製廠衊積 ~ 醖窪醖簾觸醖糧淵築選) 更多	-	2020-06-09
NCT02328027 (CTgov)	临床1/2期	类风湿关节炎 \| 强直性脊柱炎	16	99mTc-rhAnnexin V-128 (99mTc-rhAnnexin V-128: Rheumatoid Arthritis)	壓齋壓簾構鑰獵醖艱繭(廠壓餘積鹹艱鹽鬱範夢) = 廠積醖餘糧繭積鏇鬱築壓繭艱廠範淵醖鏇構壓 (廠夢網築膚鹽夢顧膚夢, 簾構衊網築築鹽窪鬱繭 ~ 鏇網艱構餘襯醖壓鹹網) 更多	-	2020-06-09
NCT03232580 (CTgov)	临床2期	脊椎关节炎	5	rhAnnexin V-128	餘構鏇積襯衊齋齋願構(選壓構鏇壓夢網壓選鹹) = 繭選觸醖憲範構蓋顧積廠鏇醖餘鬱繭衊鹹窪醖 (衊願遞範鏇鹹膚簾願願, 蓋膚憲遞糧觸鑰繭觸壓 ~ 構觸遞鏇簾顧襯顧襯壓) 更多	-	2019-12-13