Tucaresol increases oxygen affinity and reduces haemolysis in subjects with sickle cell anaemia

Arya, Roopen; Rolan, P.; Wootton, R.; Posner, John; Bellingham, A. J.

doi:10.1046/j.1365-2141.1996.d01-1744.x

Cited by 48 publications

(53 citation statements)

References 14 publications

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“…Tucaresol has proved effective against experimental models of cytomegalovirus and murine colon adenocarcinoma and has been shown to be biologically active as an immunopotentiator, favoring a Th1 response in patients with malignant melanoma (29,36). Tucaresol was well tolerated at doses of 400 mg/kg of body weight in phase I and II melanoma trials (29), and an elimination half-life of 1 week was shown in other studies (4). The costimulatory potential of tucaresol, as well as its ability to bias immunity toward a cellmediated T-helper-cell response, suggests that it could prove to be of therapeutic benefit against chronic infectious diseases such as VL, which is characterized by its ability to induce T-cell anergy (26).…”

mentioning

confidence: 99%

Activity of the Novel Immunomodulatory Compound Tucaresol against Experimental Visceral Leishmaniasis

Smith

Yardley

Rhodes³

et al. 2000

Antimicrob Agents Chemother

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Tucaresol, a novel immunomodulator, was inactive against Leishmania donovani amastigotes in both peritoneal and bone marrow macrophages in vitro at concentrations between 100 and 1 M, with toxicity to macrophages and parasites at 300 M. However, against L. donovani in BALB/c mice at doses between 80 and 1.25 mg/kg of body weight administered once daily by the oral route during days 7 to 11 of infection, an optimal dose of 5 mg/kg produced a 43.8 to 62.4% suppression of liver amastigotes, with significantly reduced activity at the extremes of the dose range. This response was not related to levels of infection. No interaction with the standard pentavalent antimonial sodium stibogluconate (Pentostam) was observed during this period of infection. The optimum dose of 5 mg/kg was ineffective when administered during the first week of infection and was most effective against the liver infection when administered during weeks 2 to 3 of infection (42.3 to 46.8% inhibition) and against the splenic infection when administered during week 6 of infection (59.5% inhibition). The optimum dose of tucaresol against L. donovani in C57BL/6 mice was 5 mg/kg, which produced a 40.8 to 48.7% suppression of liver amastigotes when administered in a range of 80 to 1.25 mg/kg during days 7 to 11 of infection. The drug had no activity against L. donovani infections in C.B-17 scid mice when the same regimen was used.

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mentioning

confidence: 99%

Activity of the Novel Immunomodulatory Compound Tucaresol against Experimental Visceral Leishmaniasis

Smith

Yardley

Rhodes³

et al. 2000

Antimicrob Agents Chemother

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“…The scientific rationale for this biomarker was based on the observation that HbS polymerization is inhibited when 20-30% of hemoglobin is maintained in the oxy-conformation. Measurements of %MOD were included in the initial phase I studies and used to guide dose tucaresol dosage in the initial patient studies (55,56).…”

Section: Biomarkers In Early (Exploratory) Phase Clinical Developmentmentioning

confidence: 99%

A Rational Approach to Drug Development: The Exploratory Phase

Ette

Garg

Jayaraj

2004

Clinical Research and Regulatory Affairs

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Drug development is a complex process, and added to it is the sophisticated new technologies and approaches to drug design, of which rational drug design is the epitome. A low success rate for investigational new drugs calls for improvement in drug discovery and development processes. Implementing knowledge driven drug development strategies founded on informative, powerful, and robust studies would greatly improve the drug discovery and development processes. Knowledge driven drug discovery and development that emphasizes a learn-confirm-learn paradigm is proposed as the rational basis for drug development. Although clinical drug development is usually divided into Phases I, II, III, and IV; it should rather be defined by those studies necessary to obtain data to answer the fundamental development decision questions: ''Is the new molecular entity tolerated and at what dose range?'' and ''Does it show efficacy for intended use within the tolerated dose range?'' In setting out to answer these questions during drug development, we propose that the learn-confirm-learn paradigm of drug development provides the most appropriate answers to these questions and hence a rational and optimal drug development process (DDP). The exploratory phase of drug development provides the Clinical Research and Regulatory Affairs Downloaded from informahealthcare.com by Kainan University on 04/08/15For personal use only.answer to the first question, and answers the second question in part through a welldesigned proof of concept study.

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“…We were also able to make accurate predictions about the likely clinical dose based on the use of this required to test this hypothesis. During the time while surrogate, as in sickle cell disease patients, %MOD levels predicted to be likely to be therapeutic were associated with substantial reductions in several haematological indices of haemolysis [23]. These tests however are also surrogates, but more closely related to the basic pathology and hence can be regarded as more proximate to the disease than %MOD.…”

Section: The Properties Of Surrogates-their 'Dimensions'mentioning

confidence: 99%

The contribution of clinical pharmacology surrogates and models to drug development—a critical appraisal

Rolan

1997

Brit J Clinical Pharma

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Tucaresol increases oxygen affinity and reduces haemolysis in subjects with sickle cell anaemia

Cited by 48 publications

References 14 publications

Activity of the Novel Immunomodulatory Compound Tucaresol against Experimental Visceral Leishmaniasis

Activity of the Novel Immunomodulatory Compound Tucaresol against Experimental Visceral Leishmaniasis

A Rational Approach to Drug Development: The Exploratory Phase

The contribution of clinical pharmacology surrogates and models to drug development—a critical appraisal

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