马立马司他(Marimastat) - 药物靶点：MMPs_专利_临床

概要

基本信息

药物类型

小分子化药

别名

Marimastat (USAN/INN)、BB 2516、BB-2516

+ [6]

靶点

MMPs

作用方式

抑制剂

作用机制

MMPs抑制剂(基质金属蛋白酶家族抑制剂)

治疗领域

肿瘤神经系统疾病消化系统疾病+ [4]

在研适应症-

非在研适应症

乳腺癌胶质瘤头颈部肿瘤+ [7]

原研机构

Merck & Co., Inc.

在研机构-

非在研机构

Mitsubishi Tanabe Pharma Corp.ILEX Oncology Services, Inc.

Merck Sharp & Dohme Corp.

+ [1]

权益机构-

最高研发阶段终止临床3期

首次获批日期-

最高研发阶段(中国)-

特殊审评-

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结构/序列

分子式C15H29N3O5

InChIKeyOCSMOTCMPXTDND-OUAUKWLOSA-N

CAS号154039-60-8

关联

4

项与马立马司他相关的临床试验

NCT00261391

/ Completed临床1期IIT

Phase I Dose Escalation Study to Evaluate the Safety and Preliminary Efficacy of Marimastat in Patients With Disabling Malformations and No Other Treatment Options

3 patients were enrolled in each of 3 study cohorts. There three cohorts were given differing, incrementally larger doses of this phase I drug. The same safety measures are being obtained on all patients. Efficacy measures were individualized as enrolllees do not have the same underlying vascular anomaly. The study is structured to include a 24 month drug-phase and a 24 month follow-up phase. The study is now closed to enrollment.

开始日期2000-10-01

申办/合作机构

The Children's Hospital Corp.

NCT00003010

/ Completed临床3期IIT

A Randomized Phase III Trial of Marimastat Versus Placebo in Patients With Metastatic Breast Cancer Who Have Responding or Stable Disease After Induction Chemotherapy

RATIONALE: Marimastat may stop the growth of breast cancer by stopping blood flow to the tumor. It is not known whether chemotherapy is more effective with or without marimastat for breast cancer.
PURPOSE: Randomized double-blinded phase III trial to compare the effectiveness of marimastat with that of no further therapy in treating women who have metastatic breast cancer that is responding or stable after chemotherapy.

开始日期1997-12-02

申办/合作机构

Eastern Cooperative Oncology Group

[+2]

NCT00003011

/ Completed临床3期IIT

A Phase III Study of Marimastat in Patients With Small Cell Lung Cancer Following a Response to First Line Chemotherapy

RATIONALE: Marimastat may stop the growth of lung cancer by stopping blood flow to the tumor. It is not yet known if marimastat is an effective treatment for small cell lung cancer.
PURPOSE: Randomized phase III trial to compare the effectiveness of marimastat with a placebo following chemotherapy in treating patients who have small cell lung cancer.

开始日期1997-01-31

申办/合作机构

NCIC Clinical Trials Group

100 项与马立马司他相关的临床结果

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100 项与马立马司他相关的转化医学

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100 项与马立马司他相关的专利（医药）

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443

项与马立马司他相关的文献（医药）

2025-06-01·JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY

Uremic Toxins, CKD, and Cognitive Dysfunction

Review

作者: Day, Gregory S. ; Irani, Sarosh R. ; Kanekiyo, Takahisa ; Hickson, LaTonya J. ; Andrews, Taylor D.

Cognitive impairment involves alterations to one's cognitive status that affects everyday life. Individuals with CKD, and particularly kidney failure, experience higher rates of cognitive impairment (20%–70%) compared with the general population. The highest prevalence is described in kidney failure such that dialysis-dependent patients have twice the prevalence of age-matched controls. In the past 5 years, the number of investigations examining the “kidney-brain axis,” mechanisms of CKD-related cognitive impairment, and potential therapeutics have exponentially increased. This review article summarizes recent literature on direct and indirect effects of CKD-associated cognitive impairment with emphasis on uremic toxins; brain injury mechanisms; overlap between CKD-associated cognitive impairment, Alzheimer's disease, and other neurodegenerative diseases. Reviewed therapeutic interventions include AST-120 (indoxyl sulfate absorbent), CH-223191 (aryl hydrocarbon receptor antagonist), triarylmethane-34 (Kca3.1-specific inhibitor), anakinra (IL-1R inhibitor), marimastat, exercise, supplements, and kidney transplantation. Special focus is placed on translational studies examining uremic toxin–associated pathogenic processes, including brain oxidative stress, neuroinflammation, and blood-brain barrier dysfunction through in vitro and in vivo models of CKD-associated brain injury. Finally, future research directions are suggested, including targeting of cellular senescence abundance with senotherapeutics and capitalizing on anti-inflammatory effects of regenerative, cell-based therapeutics (e.g., mesenchymal stem cells and extracellular vesicles), and use of aged murine models. Collectively, CKD-associated cognitive impairment represents a prevalent condition for which remaining knowledge gaps exist, and scientific advancements are needed to preserve cognitive function and improve the lives of individuals with CKD.

2025-06-01·BIOCHEMICAL PHARMACOLOGY

Therapeutic opportunities in polycystic kidney and liver disease through extracellular matrix dynamics

Article

作者: Bravo, Susana ; Lamas-González, Olaya ; Nuñez-González, Laura ; Cordido, Adrian ; García-González, Miguel A ; Banales, Jesus M ; Vizoso-González, Marta ; Díaz, Candido

Autosomal Dominant and Autosomal Recessive Polycystic Kidney Disease (ADPKD and ARPKD) are, respectively, common and rare forms of polycystic disorders, characterized by the formation and progressive growth of cysts from tubules in the kidneys and bile ducts in the liver. Alterations in the extracellular matrix (ECM) and in the activity of matrix metalloproteases (MMPs), both associated with fibrosis, have been shown to be important factors in cystic growth and progression of these diseases. We used tandem mass spectrometry (LC-MS/MS) to identify the most enriched proteins and pathways in an orthologous rapidly progressive mouse model of ADPKD: Pkd1^flox/floxTamCre. This information was used to discover and validate novel therapeutic targets in orthologous models of ADPKD (Pkd1^flox/floxTamCre) and ARPKD (Pkdh1^{del3-4/del3-4}). ECM related pathways and expression levels of MMPs were among the most dysregulated cellular processes in polycystic kidney and liver. Selective inhibition of MMPs by marimastat (MTT) altered the ECM response and resulted in inhibition of collecting duct-derived cyst growth, delay of global kidney cyst progression and rescue of liver phenotype by normalized MMPs expression and significant reduction in fibrosis. This phenotypic improvement was further enhanced by treatment of MTT and tolvaptan, indicating an additive benefit to targeting the fibrotic and growth pathways in cysts. As conclusion, targeting of MMPs are important in ECM dysregulation and offers a new potential therapeutic strategy for both kidney and bile duct derived fibrocystic disease in ADPKD and ARPKD. Such approaches can have additive benefits with other treatment approaches, such as tolvaptan.

2025-05-01·Cancer Medicine

Inside a Metastatic Fracture: Molecular Bases and New Potential Therapeutic Targets

Review

作者: Zunarelli, Renato ; Fiore, Michele ; Sambri, Andrea ; Cappelli, Alberta ; Bruschi, Alessandro ; Scollo, Cristina ; Di Prinzio, Lorenzo ; Pace, Andrea ; Montanari, Andrea ; Bubbico, Elisa ; De Paolis, Massimiliano

ABSTRACT:

Introduction:

Bone metastases and pathological fractures significantly impact the prognosis and quality of life in cancer patients. However, clinical and radiological features alone have been shown to fail to predict skeletal related events of a bone metastasis (SREs).

Aim:

This study focuses on key molecular players including Matrix Metalloproteinases (MMPs), Integrins, Bone Morphogenetic Proteins (BMPs), Parathormone‐related Protein (PTHrP).

Results:

The RANK/RANKL/Osteoprotegerin (OPG) pathway, and N‐terminal peptide (NTx), involved in the metastatic process and bone integrity disruption. Elevated levels of these molecules have been pointed out as potential biomarkers for predicting SREs, but they have been poorly investigated. Moreover, batimastat, marimastat, tanomastat, andecaliximab, and HIV protease targeting MMPs; Volociximab/M200, cilengitide, abituzumab, and FAK inhibitors targeting integrins; LDN193189, DMH1, and ISLR modulators targeting BMPs; and PTH (7–33)‐CBD targeting PTHrP have shown promising results antagonizing these molecules, but no effect on preventing and managing metastatic fractures has been assessed yet.

Conclusions:

This paper underscores the importance of advanced molecular biology and transcriptomics in identifying novel therapeutic targets. The integration of these biomarkers with clinical and radiological assessments using artificial intelligence tools could revolutionize the diagnostics and treatment strategies for patients with bone metastases.

100 项与马立马司他相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D03795	马立马司他	-	DB00786

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
小细胞肺癌	临床3期	加拿大	NCIC Clinical Trials Group	1997-01-31
非小细胞肺癌 III期	临床3期	美国	ILEX Oncology Services, Inc.	1996-12-01
非小细胞肺癌 III期	临床3期	加拿大	ILEX Oncology Services, Inc.	1996-12-01
乳腺癌	临床3期	美国	-	-
胶质瘤	临床3期	美国	-	-
胶质瘤	临床3期	欧盟	-	-
胶质瘤	临床3期	加拿大	-	-
肺癌	临床3期	-	Merck Sharp & Dohme Corp.	-
卵巢癌	临床3期	美国	-	-
卵巢癌	临床3期	欧盟	-	-

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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


E2196 (Pubmed \| J Clin Oncol)	临床3期	转移性乳腺癌一线	-	Marimastat	願網淵醖網築鬱壓製築(獵鑰壓齋簾選網構遞網) = Patients with grade 2 or 3 MST had significantly inferior survival compared with patients who had grade 0 or 1 MST (median, 22.5 months v 28.2 months; P = .04) 壓獵網廠齋簾遞構鬱壓 (夢餘簾蓋繭觸壓膚製顧 ) 更多	不佳	2004-12-01
				Placebo
NCT00003011 (Pubmed \| J Clin Oncol)	临床3期	小细胞肺癌辅助	532	Marimastat 10 mg	遞鹹夢顧鑰鏇壓觸蓋築(膚遞壓築憲選廠窪糧壓) = 醖憲繭憲築鹹觸遞壓壓艱製餘鏇餘蓋網鏇製鏇 (構夢範鏇鏇鬱膚築鬱鹹 ) 更多	不佳	2002-11-15
				Placebo	遞鹹夢顧鑰鏇壓觸蓋築(膚遞壓築憲選廠窪糧壓) = 獵鹹衊遞衊窪壓鏇鏇觸艱製餘鏇餘蓋網鏇製鏇 (構夢範鏇鏇鬱膚築鬱鹹 ) 更多