This trial evaluates primary care clinic-based simplified antibiotic therapy options for young infants, 0-59 days old in high neonatal mortality settings in peri-urban Karachi where hospital referral is frequently refused by families.

开始日期2009-12-01

申办/合作机构

Aga Khan University

[+4]

NCT00189384 / Unknown status临床3期IIT

Randomized Controlled Trial of Intramuscular Ceftriaxone Versus Procaine Penicillin Versus Cotrimoxazole and Gentamicin for Management of Serious Bacterial Infections in Young Infants in Community Settings

Approximately one-third of neonatal deaths in developing countries are due to infections acquired through the birth canal and/or exposure to an unclean environment soon after birth. Current World Health Organization recommendations for the management of infants younger than 2 months of age who have serious bacterial infections involve hospitalization and parenteral therapy for at least 10 days with antibiotic regimens containing penicillin or ampicillin combined with an aminoglycoside.However, in many settings throughout the developing world, this is not currently possible, nor is this standard of care likely to be feasible in the near future. Several studies have reported that for a variety of sociocultural reasons many families are unable or unwilling to access hospital-based care and their sick young infants do not get hospitalized, and instead, receive a variety of home-based antibiotic therapies, or none at all. In our community field sites, approximately 70% of families refuse hospital referral for a sick newborn, despite provision of transport.
Thus, there is an urgent need to define the role of community/first-level facility-based care versus hospitalization for the management of young infants with serious bacterial infections, and the potential for community-based parenteral antibiotics as an alternative strategy in resource poor areas with high neonatal mortality rates. Bang and colleagues have demonstrated significant reductions in neonatal mortality from infections in an underdeveloped rural district in Maharashtra, India by a field-based case management approach which used oral cotrimoxazole and intramuscular gentamicin given for 7 days as treatment for neonates with sepsis.
This study is an equivalence randomized controlled trial (RCT) comparing once daily IM ceftriaxone injection to once daily IM procaine penicillin and gentamicin injection, to once daily intramuscular gentamicin injection and twice daily oral cotrimoxazole, given for 7 days in babies with clinically-diagnosed possible serious bacterial infection (pneumonia, or sepsis with or without local infections such as skin or umbilical infections) whose families refused referral to a hospital. After supplementary informed consent, patients meeting specific inclusion and exclusion criteria are randomly allocated to one of the three regimens being tested. The study hypothesis is that all 3 regimens will perform equally well in the treatment of sepsis in a first-level facility setting.

开始日期2003-11-01

申办/合作机构

Aga Khan University

100 项与青霉素G普鲁卡因相关的临床结果

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100 项与青霉素G普鲁卡因相关的转化医学

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100 项与青霉素G普鲁卡因相关的专利（医药）

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1,040

项与青霉素G普鲁卡因相关的文献（医药）

2024-12-01·JOURNAL OF ETHNOPHARMACOLOGY

Effect of single and combination therapy on methanol extracts of Khaya senegalensis stem bark, Vernonia amygdalina leaves and Garcinia kola seed in Leptospira interrogans-infected mice

Article

作者: Abiayi, Elmina Abiba ; Jolayemi, Kelvin Olutimilehin ; Itelima, Janet Uchechukwu ; Forcados, Gilead ; Udechukwu, Collins Chimezie ; Agida, George ; Abiayi, Daniel Chibuzo ; Abiayi, David Chinedu ; Onwuliri, Festus Chukwuemeka

ETHNOPHARMACOLOGICAL RELEVANCE:

Pastoralists in Nigeria mix Garcinia kola seed (GK), Khaya senegalensis stem bark (KS), and Vernonia amygdalina leaves (VA) to treat leptospirosis.

AIM:

To determine the in vitro and in vivo effect on single and combination therapy on Leptospira interrogans-infected mice.

MATERIALS AND METHODS:

Evaluation of in vitro assay for anti-leptospiral motility of the extracts was carried out in triplicates. For the in vivo assessment, 40 adult male mice inoculated with Leptospira were randomly allocated into 8 groups of 5 mice each. Groups IV-IX were treated with 800 mg/kg b.w. of KS, GK, VA, KS + GK, KS + VA, GK + VA for 5 days. Group I was negative control, II was model control, and III was treated with penicillin (3.7 mg/kg b.w.) intramuscularly.

RESULTS:

In vitro, at 90 min, all the extracts at 800, 400, and 200 mg/ml showed complete cessation of motility which was significantly (p < 0.05) different when compared to the negative control. A significant (p < 0.05) IC₅₀ of 0.18 mg/ml was recorded with GK when compared to KS (0.40 mg/ml), VA (0.25 mg/ml), and procaine penicillin (0.31 mg/ml). Mean packed cell volume, haemoglobin concentration, and mean corpuscular haemoglobin concentration decreased significantly (p < 0.05) in all infected groups and returned to almost pre-infection values. However, significant leucocytosis (p < 0.05) was observed in group II. AST and ALP showed a significant increase (p < 0.001). Histopathological evaluation showed the extracts to prevent the distortion of normal architecture of the selected organs.

CONCLUSION:

This study demonstrates the significant potential of Garcinia kola, Khaya senegalensis, and Vernonia amygdalina extracts singly and in combination to combat leptospirosis.

2023-10-01·Journal of equine veterinary science

Effect of Procaine Penicillin G and Flunixin Meglumine on Serum Amyloid A Response in Healthy Adult Horses

Article

作者: Pusterla, Nicola ; Nottle, Bridget F ; Trsan, Jurica

This study was designed to determine the effect of PPG and/or flunixin meglumine on SAA response when used at clinical dosing regimens in healthy adult horses. Six healthy adult horses were enrolled in a crossover study design including one control and three treatment groups: no treatment (control); PPG alone (intramuscularly q12h for 72h); flunixin meglumine alone (intravenously q24h for 72h); and PPG (intramuscularly q12h for 72h) and flunixin meglumine (intravenously q24h for 72h). Whole blood was collected at 0, 24, 48, 72, 96 and 120 hours post-initial drug administration to measure SAA using a commercial lateral-flow immunoassay. The washout period was 30 days. Individual SAA values were within the reference range (≤ 20 µg/mL) for almost all horses in the control group. One control horse displayed a SAA value of 28 µg/mL at 72 hours. All horses from the PPG group showed normal SAA values throughout the study. Apart from one horse (SAA of 24 µg/mL at 96 hours) from the flunixin meglumine group, all horses showed normal SAA values. For the PPG and flunixin meglumine group, 5 horses had SAA values within reference range. One horse displayed increased SAA values (32-45 µg/mL) between 48 to 96 hours post-drug administration. There was no difference in area under the SAA time curve amongst control and treatment groups (P > 0.05). The administration of intramuscular PPG and/or intravenous flunixin meglumine does not trigger an inflammatory response that induces a SAA value above reference range in most adult healthy horses.

2023-09-01·Equine veterinary journal

Acute phase protein concentrations following serial procaine penicillin G injections in horses

Article

作者: Gordon, Danielle L. ; Fan, Timothy M. ; Foreman, Jonathan H. ; Connolly, Sara L. ; Barger, Anne M. ; Schnelle, Amy N.

Abstract:

Background:

Acute phase protein (APP) measurement is used to detect inflammation. Intramuscular (IM) injections could cause tissue injury and induce an acute phase response (APR).

Objectives:

To evaluate the effects of IM procaine penicillin G (PPG) injections on APP concentrations in horses.

Study design:

Prospective longitudinal design.

Methods:

PPG was administered intramuscularly to six horses, twice daily, for 5 days. Plasma fibrinogen (FIB), serum amyloid A (SAA), haptoglobin (HAP), creatine kinase (CK), and aspartate aminotransferase (AST) were quantified daily for 5 days before the first injection, during the course of administration, and for 4 days after the final dose. Analytes were quantified every other day for the remaining 16 days. Data were compared using a parametric or non‐parametric repeated measures ANOVA and a Tukey's or Mann–Whitney rank sum test, respectively. Significance was set at p < 0.05.

Results:

CK was increased over baseline (mean ± SD: 200 ± 74 IU/L) on Days 1–6 (p < 0.001 to p = 0.02, mean ± SD: 723–1177 ± 355–544 IU/L) and AST was increased above baseline (mean ± SD: 233 ± 58 IU/L) on Days 2–7 and 10 (p < 0.001 to p = 0.05, mean ± SD: 307–437 ± 79–146 IU/L). Increased FIB was noted over baseline (mean ± SD: 177 ± 30 mg/dl) on Days 6–8 and 10 (p = 0.02 to p = 0.03, mean ± SD: 234–252 ± 33–49 mg/dl). SAA was increased above baseline (mean ± SD: 4.7 ± 2.9) on Day 6 (p = 0.02, mean ± SD: 113 ± 186 μg/ml). There was no change in HAP.

Main limitations:

Healthy horses were used, small sample size, and a lack of a negative control group.

Conclusions:

Serial intramuscular procaine penicillin G (IM PPG) injections may result in increased positive APP concentrations in horses and this must be considered when these test results are interpreted.

项与青霉素G普鲁卡因相关的新闻（医药）

2023-04-03

·Firstwordpharma

CMS trims first list of drugs tapped for inflation fines

The US Centers for Medicare and Medicaid Services (CMS) has quietly updated the list of Part B prescription medicines subject to penalties because their prices rose faster than the rate of inflation. In an update late last week, the agency cut seven medicines from its original list of 27 that was unveiled on March 15.A provision in the Inflation Reduction Act (IRA), which came into force last year, penalises pharmaceutical companies for charging prices that go up faster than inflation for people with disabilities or those 65 and older who are on the government's Medicare health programme (for more, see ViewPoints: Inflation Reduction Act's myriad impacts to reverberate across pharma). The move is expected to lower out-of-pocket costs for some Medicare recipients by between $1 and $372 per average dose, as of April 1, depending on their individual coverage, according to an agency press release updated on March 30.Gilead cell therapies knocked off The seven drugs that have been cut from the original list include Gilead Sciences' CAR-T therapies Yescarta (axicabtagene ciloleucel) and Tecartus (brexucabtagene autoleucel); Stemline Therapeutics' Elzonris (tagraxofusp-erzs) used for blastic plasmacytoid dendritic cell neoplasm; Shionogi's Fetroja (cefiderocol), an antibiotic to treat complicated urinary tract infections; Arcotech Biopharma's Folotyn (pralatrexate) for relapsed or refractory peripheral T-cell lymphoma; Kamada's WinRho SDF (Rhₒ(D) immune globulin) to boost platelet counts in order to prevent excessive haemorrhage; and Bausch + Lomb's Xipere (triamcinolone acetonide), which is prescribed for macular oedema associated with uveitis.CMS did not give a reason for why the original list was scaled back. Other products that remain include all five Pfizer drugs that were on the original list, namely Atgam (antithymocyte globulin equine), Bicillin L-A (penicillin G benzathine), Bicillin C-R (penicillin G benzathine and penicillin G procaine), Fragmin (dalteparin) and Nipent (pentostatin), as well as Johnson & Johnson's Rybrevant (amivantamab). Companies whose products have been flagged will be required to pay Medicare the difference in the form of a rebate ranging from roughly 14% to 20%. Meanwhile, CMS has said that by September 1, it plans to publish the first 10 Medicare Part D drugs that will be subject to government price negotiations starting in 2026.

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100 项与青霉素G普鲁卡因相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D02461	青霉素G普鲁卡因	J01CE09	DB09320

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适应症	国家/地区	公司	日期
牙龈炎	澳大利亚	Viatris Pty Ltd.	2017-08-04
淋病	澳大利亚	Viatris Pty Ltd.	2017-08-04
咽炎	澳大利亚	Viatris Pty Ltd.	2017-08-04
肺炎球菌感染	澳大利亚	Viatris Pty Ltd.	2017-08-04
呼吸道感染	澳大利亚	Viatris Pty Ltd.	2017-08-04
猩红热	澳大利亚	Viatris Pty Ltd.	2017-08-04
皮肤和皮肤结构感染	澳大利亚	Viatris Pty Ltd.	2017-08-04
葡萄球菌感染	澳大利亚	Viatris Pty Ltd.	2017-08-04
链球菌感染	澳大利亚	Viatris Pty Ltd.	2017-08-04
梅毒	澳大利亚	Viatris Pty Ltd.	2017-08-04
细菌感染	美国	King Pharmaceuticals LLC	1948-04-26