3 Arm Open-label Randomized Multidose Study of Pharmacokinetics, Safety & Tolerability of Testosterone Enanthate Administered Subcutaneously Via an Auto-injector Device or Intramuscular Testosterone Enanthate in Hypogonadal Adult Males

Relative Bioavailability and Safety comparison of 3 formulations of Testosterone Enanthate.

开始日期2013-09-30

申办/合作机构

Antares Pharma, Inc.

NCT01122342 / Suspended临床1/2期IIT

Vaginal Testosterone Cream For Atrophic Vaginitis in Women Taking Aromatase Inhibitors for Breast Cancer.

Atrophic vaginitis is a condition in which the skin lining of the vagina and labia becomes thin and symptoms develop including vaginal itching, vaginal discomfort and dyspareunia. These can significantly affect women's comfort, sexuality and quality of life.
Treatment for this condition includes estrogen given in pill form, commonly known as hormone replacement therapy and local estrogen treatments, such as vaginal estrogen creams and topical vaginal lubricants. Unfortunately, systemic estrogen is contraindicated in many women with breast cancer. Some providers also feel that women who are taking aromatase inhibitors for their breast cancer should also not use local estrogens as several small studies suggest that these treatments might effect estrogen levels and thus might change how effective the aromatase inhibitors are. If these women choose not to use any form of estrogen therapy there symptoms may not be well controlled with other treatments.
The investigators hypothesize that a vaginal testosterone cream might be a safe and effective alternative treatment for these women. This small study is intended to test the hypothesis that testosterone cream will not increase estrogen (estradiol) levels and that it will improve the symptoms of atrophic vaginitis including vaginal dryness, vaginal itching and pain with intercourse.
The investigators will enroll women in the trial who are taking an aromatase inhibitor and have the symptoms mentioned above. They will receive a testosterone cream which will be applied vaginally once a day for 28 days. If good results are found with a prespecified dose of testosterone, a lower dose will be tested in the next group of women enrolled.

开始日期2006-12-01

申办/合作机构

University of Vermont

100 项与丙酸睾酮相关的临床结果

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100 项与丙酸睾酮相关的转化医学

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100 项与丙酸睾酮相关的专利（医药）

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4,735

项与丙酸睾酮相关的文献（医药）

2024-01-03·Journal of toxicology and environmental health. Part A

Evaluation of the anti-androgenic and cytotoxic effects of benzophenone-3 in male Sprague-Dawley rats.

Article

作者: Chi Rim Sung ; Byeong Jun Kim ; Chan Ju Park ; In Ah Oh ; Yu Jin Lee ; Yeo Rim Park ; Seung Jun Kwack

Benzophenone-3 (BP-3, 2-hydroxy-4-methoxybenzophenone, oxybenzone) is one of the most widely used types of benzophenone organic sunscreen. However, this compound is a potentially harmful toxicant. The aim of this study was 2-fold to: (1) utilize a Hershberger bioassay in vivo in castrated male Sprague-Dawley rats to investigate the anti-androgenic activities of BP-3, and (2) use in vitro a methyl tetrazolium assay to compare the toxicity between Leydig cells (TM3 cells) and mouse fibroblast (NIH-3T3) cell lines. In the Hershberger assay, rats were divided into 6 groups (each of n = 7): a vehicle control, negative control, positive control, PB-3 low (40 mg/kg), BP-3 intermediate (200 mg/kg), and BP-3 high (1000 mg/kg)-dose. The weight of the ventral prostate was significantly decreased at BP-3 doses of 200 or 1,000 mg/kg/day. In addition, the levator anibulbocavernosus muscle weights were also significantly reduced at BP-3 doses of 40, 200, or 1,000 mg/kg/day. In the MTT assay, the viability of NIH-3T3 mouse fibroblast cells was within the normal range. However, the TM3 mouse testis Leydig cell viability was significantly lowered in a concentration-dependent manner. Therefore, data indicate that BP-3 might exert in vivo anti-androgenic and in vitro cytotoxic effects in cells associated with the male reproductive system compared to normal non-reproductive cells.Abbreviation: BP-3: benzophenone-3; CG: Cowper's gland; DMEM: Dulbecco's modified Eagle's medium; DMSO: dimethyl sulfoxide; GP: glans penis; LABC: levator anibulbocavernosus muscle; MTT: methyl tetrazolium; NC: negative control; PC: positive control; SV: seminal vesicle; TP: testosterone propionate; VC: vehicle control; VP: ventral prostate.

2023-12-27·Cells

Reduction in Nuclear Size by DHRS7 in Prostate Cancer Cells and by Estradiol Propionate in DHRS7-Depleted Cells.

Article

作者: Andrea Rizzotto ; Sylvain Tollis ; Nhan T Pham ; Yijing Zheng ; Maria Alba Abad ; Jan Wildenhain ; A Arockia Jeyaprakash ; Manfred Auer ; Mike Tyers ; Eric C Schirmer

Increased nuclear size correlates with lower survival rates and higher grades for prostate cancer. The short-chain dehydrogenase/reductase (SDR) family member DHRS7 was suggested as a biomarker for use in prostate cancer grading because it is largely lost in higher-grade tumors. Here, we found that reduction in DHRS7 from the LNCaP prostate cancer cell line with normally high levels of DHRS7 increases nuclear size, potentially explaining the nuclear size increase observed in higher-grade prostate tumors where it is lost. An exogenous expression of DHRS7 in the PC3 prostate cancer cell line with normally low DHRS7 levels correspondingly decreases nuclear size. We separately tested 80 compounds from the Microsource Spectrum library for their ability to restore normal smaller nuclear size to PC3 cells, finding that estradiol propionate had the same effect as the re-expression of DHRS7 in PC3 cells. However, the drug had no effect on LNCaP cells or PC3 cells re-expressing DHRS7. We speculate that separately reported beneficial effects of estrogens in androgen-independent prostate cancer may only occur with the loss of DHRS7/ increased nuclear size, and thus propose DHRS7 levels and nuclear size as potential biomarkers for the likely effectiveness of estrogen-based treatments.

2023-12-01·Bone reports

Bone strength is reduced in a neonatal androgenized rat model.

Article

作者: Lady Katerine Serrano Mujica ; Carolina Dos Santos Amaral ; Fernanda Soldatelli Valente ; Ligia Gomes Miyazato ; Soraia Macari ; Tarcília Aparecida da Silva ; Breno Rocha Barrioni ; Bruna Leonel Carlos ; Guilherme Jafroni Alves Silva ; Antônio Carlos Shimano ; Alfredo Quites Antoniazzi ; Melissa Orlandin Premaor ; Fabio Vasconcellos Comim

Background:

Whether polycystic ovary syndrome (PCOS) affects bone health during a woman's lifespan remains controversial. An androgenized rodent model replicated many metabolic and reproductive features of women with PCOS, and we aimed to use it to investigate the impact of androgens on microarchitecture (by micro-CT), bone mechanical strength, bone formation and resorption markers in rats with intact ovaries (SHAM) who underwent oophorectomy.

Methods:

Wistar rats (Rattus norvegicus albinus) were employed for the experiments in this study. The protocol of androgenization consisted of the application of 1.25 mg s.c. testosterone propionate beteween days 2-5 of life, while the controls received the same amount of corn oil s.c. as previously established. Androgenized SHAM rats exhibited chronic anovulation identified by vaginal cytology and a reduction in the proportion of corpus luteum in the ovary in comparison to control SHAM rats. The realization of the ovariectomy or SHAM procedure occurred on Day 100 of life. All groups (n = 8) were followed-up for 180 days to address the study endpoints.

Results:

Micro-CT from androgenized female rats (SHAM) showed a divergence between the trabecular and cortical bone profiles. Compared to SHAM controls, these rats had an increase in trabecular bone mass with a diminution in bone resorption C-terminal telopeptide of type 1 collagen (CTX) (p < 0.05), a concomitant decrease in cortical area and thickness in the femur, and a reduction in the strength of the femur on the mechanical test (p < 0.01).

Conclusions:

Our results suggest that a reduction in the cortical thickness and cortical area observed in PCOS model rats was associated with a reduced strength of the femur, despite increased trabecular formation. Ovariectomy in the androgenized OVX group limited the progression rate of cortical bone loss, resulting in bone resistance and cortical thickness comparable to those observed in the control OVX group.

项与丙酸睾酮相关的新闻（医药）

2023-02-15

·蒲公英Ouryao

3.4万瓶！仿制药被召回！

转自：蒲公英Ouryao 整理：青于蓝根据美国FDA最近的一份执法报告，太阳药业Halol工厂生产的某些批次的仿制盐酸地尔硫卓缓释胶囊未能通过FDA实验室的稳定性检测和溶出度测试。太阳药业于2023年1月13日开始召回，召回归类为2级召回（2级召回是指可能导致暂时性不良健康后果或极有可能造成严重健康后果的情况）。未能通过FDA实验室的稳定性检测和溶出度测试根据美国FDA最近的一份执法报告，太阳药业Halol工厂正在自愿召回3.4万瓶仿制盐酸地尔硫卓，原因是在FDA实验室执行的稳定性测试中杂质（脱乙酰地尔硫卓盐酸盐）标准不合格，且未通过溶解度检测。盐酸地尔硫卓用于治疗高血压、胸痛和某些心律失常。根据FDA的报告，太药药业正在自愿召回3.4万瓶仿制盐酸地尔硫卓，原因是在FDA实验室执行的稳定性测试中杂质（脱乙酰地尔硫卓盐酸盐）标准不合格，且未通过溶解度检测。太阳药业于2023年1月13日开始召回，FDA将召回归类为2级召回。太阳药业Halol工厂多次被召回2022年6月，太阳药业Halol工厂因漏水而主动召回50,680瓶环戊丙酸睾酮注射液。2016年8月印度太阳制药Halol工厂召回美国与波多黎各市场价值381,120卢比的阿伦膦酸钠（阿仑膦酸钠/阿屈膦酸钠）。太阳制药Halol工厂生产的该药在3个月的稳定性试验中即被检测到未知杂质超出规定限度。此次召回也是属于2类召回。2012年3月，太阳制药Halol工厂从美国召回15.5万瓶滴眼液，该滴眼液用于缓解解结膜炎。这次也是因其杂质超限。每年483报告不离手除了产品召回外，太阳药业Halol工厂还多次收到FDA警告信：2022年5月份 , FDA发布了一封 483 报告。在2014 年和 2015 年分别对其发布了两封警告信，并在过去五年里发布了不下十封 483。参考：识林药渡

2023-02-10

·PRNewswire

Kintor Pharma Announces Positive Top-line U.S. Phase I Trial Results of GT20029, the World's First Topical Use PROTAC Compound

SUZHOU, China, Feb. 10, 2023 /PRNewswire/ -- Kintor Pharmaceutical Limited ("Kintor Pharma", HKEX: 9939), a clinical-stage biotechnology company developing innovative small molecules and biological therapeutics, announced the positive top-line results from the U.S. Phase I clinical trial of GT20029, a Kintor Pharma in-house developed and fully owned proteolysis targeting chimera (PROTAC) compound. The data showed GT20029 was safe, well tolerated and had good pharmacokinetic characteristics in healthy subjects as well as subjects with androgenetic alopecia (AGA) or acne. GT20029 is the first topical PROTAC compound in the world which has completed Phase I clinical trial in both China and the U.S.. This is a randomized, double-blind, placebo-controlled, parallel group, dose escalation Phase I clinical study to evaluate the safety, tolerability and pharmacokinetics of GT20029 following topical single ascending dose administration (SAD) in healthy subjects and multiple ascending dose administration (MAD) in subjects with AGA or acne. The results showed that GT20029 was safe and well tolerated at all dose levels in all cohorts. No treatment-emergent adverse events (TEAEs) related to GT20029 in the SAD stage were reported. The most common TEAEs in the MAD stage were mild, including dryness, itching, burning and pain at application site. No serious adverse events (SAEs) were reported. No severe (Grade ≥3) TEAEs and no subject withdrawal or death caused by TEAEs were reported. In the SAD stage, subjects had no systemic exposure at all dose levels, and all sample concentrations were below the lower limit of quantification (LLOQ, 0.003ng/mL). In the MAD stage, after 14 days of continuous administration in subjects with AGA or acne, the systemic exposure was very limited and the mean maximum observed concentration (Cmax) of all dose levels fluctuated near the LLOQ, with the highest not exceeding 0.015 ng/mL. In preclinical studies, by degrading androgen receptor (AR) protein, GT20029 could block the shrinkage and miniaturization of hair follicles which was caused by the activation of AR signaling pathway. As the result, it prevented the hair from thinning, softening and falling out. GT20029 could also effectively inhibit sebaceous gland development and sebum secretion. With limited skin penetration, GT20029 could avoid high systemic exposure and achieve a better safety profile. The repeated pharmacodynamics studies in dihydrotestosterone (DHT)-induced mouse model showed that GT20029 significantly promoted hair growth, with statistical difference. The study of testosterone propionate (TP)-induced skin hamster flank organ acne model showed that GT20029 significantly inhibited enlargement of flank organ, with statistical difference. Dr. Youzhi Tong, founder, Chairman and Chief Executive Officer of Kintor Pharma, commented, "The positive U.S. Phase I top-line results of GT20029 in 123 subjects has shown a similar result with that of Phase I trial in China with 92 subjects enrolled. Both studies have demonsrtated the good safety and tolerability in MAD of GT20029. Alopecia affects about 1.6 billion people and acne affects about 0.72 billion people worldwide, there are huge unmet clinical needs. We will accelerate the initiation of Phase II clinical trial of GT20029, maintain our leading position in the development of topical PROTAC drug candidate globally. We believe that GT20029 would strengthen our market position in the dermatology area, together with our novel drug KX-826, to provide a diversified portfolio of therapies to patients with AGA or acne. " About GT20029 GT20029 is a topical AR degrader developed by Kintor Pharma's PROTAC platform. The China National Medical Products Administration (NMPA) and the U.S. Food and Drug Administration (FDA) cleared GT20029's clinical trial applications for treating AGA and acne in April 2021 and July 2021, respectively. In August 2022, Kintor Pharma had completed the enrollment and dosing of subjects for its China Phase I clinical trial. In November 2022, Kintor Pharma announced the top-line results for its China Phase I clinical trial. In October 2022, Kintor Pharma announced completion of subject enrollment and dosing in its U.S. Phase I clinical trial. About Kintor Pharmaceutical Limited Kintor Pharmaceutical Limited is developing and commercializing a robust pipeline of innovative small molecule and biological therapeutics for androgen-receptor-related disease areas with unmet medical needs, including COVID-19, prostate, breast and liver cancers, alopecia and acne. For more information, visit . SOURCE Kintor Pharma

临床1期临床结果临床申请

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KEGG	Wiki	ATC	Drug Bank
D00959	丙酸睾酮	G03BA03	DB01420

研发状态

适应症	最高研发状态	国家/地区	公司
低睾酮水平	批准上市	美国更多	Acerus Pharmaceuticals Corp. 更多
青春期延迟	批准上市	意大利更多	-
更年期综合症	批准上市	英国更多	-
乳腺癌	批准上市	意大利更多	-
性腺机能减退	批准上市	美国更多	Acerus Pharmaceuticals Corp. 更多

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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


NCT01887418 (CTgov)	临床1/2期	性腺机能减退	39	QuickShot™ - 100 mg Treatment A (QuickShot™ - 100 mg Treatment A)	(壓獵壓繭願艱膚積壓鏇) = 鏇糧醖鏇構觸餘蓋壓顧繭憲選醖蓋衊醖簾蓋鹽 (選淵遞簾積鹹鑰憲選鹽, 鏇築構夢構餘鹹窪簾齋 ~ 觸鬱鬱築膚遞醖壓構構) 更多	-	2015-10-21
NCT01887418 (CTgov)	临床1/2期	性腺机能减退	39	QuickShot™ - 50 mg Treatment B (QuickShot™ - 50 mg Treatment B)	(壓獵壓繭願艱膚積壓鏇) = 憲觸憲繭繭觸襯簾鏇觸繭憲選醖蓋衊醖簾蓋鹽 (選淵遞簾積鹹鑰憲選鹽, 範選願顧顧鹹齋醖遞簾 ~ 網觸襯窪夢夢築鹹餘願) 更多	-	2015-10-21
NCT04424654 (PSMA-BAT, ESMO2023) 人工标引	临床2期	转移性去势抵抗性前列腺癌	20	testosterone 400 mg	(窪襯憲鹹繭憲觸蓋顧簾) = 範餘遞鏇獵鬱窪繭餘繭淵積顧壓構醖鑰壓鏇築 (鏇獵鏇憲繭繭範顧壓鏇 ) 更多	积极	2023-10-22