PCTH: a novel orally active chelator of the aroylhydrazone class that induces iron excretion from mice

IF 4.2 2区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Biochimica et biophysica acta. Molecular basis of disease Pub Date : 2004-12-24 DOI:10.1016/j.bbadis.2004.09.001

C.S.M. Wong, J.C. Kwok, D.R. Richardson

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Abstract

β-Thalassaemia major is an inherited blood disorder which is complicated by repeated blood transfusion and excessive gastrointestinal iron (Fe) absorption, which leads to toxic Fe overload. Current treatment using the chelator, desferrioxamine (DFO), is expensive and cumbersome since the drug requires long subcutaneous infusions and it is not orally active. A novel chelator, 2-pyridylcarboxaldehyde 2-thiophenecarboxyl hydrazone (PCTH), was recently designed and shown to have high Fe chelation efficacy in vitro [E.M. Becker, D.R. Richardson, J. Lab. Clin. Med. 134 (1999) 510–521; D.R. Richardson, et al., Biochim. Biophys. Acta 1536 (2001) 133–140]. The aim of this investigation was to examine the Fe chelation efficacy of PCTH in vitro implementing primary cultures of cardiomyocytes and in vivo using mice. We showed that PCTH was significantly (P<0.005) more effective than DFO at mobilising ⁵⁹Fe from prelabelled cardiomyocytes. Moreover, PCTH prevented the incorporation of ⁵⁹Fe into ferritin during Fe uptake from ⁵⁹Fe-labelled transferrin. These effects were important to assess as cardiac complications caused by Fe deposition are a major cause of death in β-thalassaemia major patients. Further studies showed that PCTH was orally active and well tolerated by mice at doses ranging from 50 to 200 mg/kg, twice daily (bd), for 2 days. A dose-dependent increase in faecal ⁵⁹Fe excretion was observed in the PCTH-treated group. This level of Fe excretion at 200 mg/kg was similar to the same dose of the orally effective chelators, pyridoxal isonicotinoyl hydrazone (PIH) and deferiprone (L1). Effective Fe chelation in the liver by PCTH was shown via its ability to reduce ferritin-⁵⁹Fe accumulation. Mice treated for 3 weeks with PCTH at doses of 50 and 100 mg/kg/bd showed no overt signs of toxicity as determined by weight loss and a range of biochemical and haematological indices. In subchronic Fe excretion studies over 3 weeks, PIH and PCTH at 75 mg/kg/bd for 5 days/week increased faecal ⁵⁹Fe excretion to 140% and 145% of the vehicle control, respectively. This study showed that PCTH was well tolerated at 100 mg/kg/bd and induced considerable Fe excretion by the oral route, suggesting its potential as a candidate to replace DFO.

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PCTH：一种新的口服活性芳基腙类螯合剂，可诱导小鼠铁排泄

β-地中海贫血是一种遗传性血液疾病，伴有反复输血和胃肠道铁（Fe）吸收过多，从而导致有毒的铁过载。目前使用螯合剂去铁胺（DFO）的治疗既昂贵又麻烦，因为该药物需要长时间的皮下输注，而且不具有口服活性。一种新型螯合剂- 2-吡啶基甲醛- 2-噻吩羧基腙（PCTH）最近被设计出来，并在体外显示出高铁螯合效果[em]dr . Richardson， J. Lab。中国。医学杂志134 (1999)510-521；dr . r . Richardson等人，《生物化学》。Biophys。学报1536(2001)133-140]。本研究的目的是在体外进行心肌细胞原代培养和小鼠体内研究PCTH对铁的螯合作用。我们发现PCTH在从预先标记的心肌细胞中动员59Fe方面明显比DFO更有效（P<0.005）。此外，在从59Fe标记的转铁蛋白摄取铁时，PCTH阻止了59Fe与铁蛋白的结合。这些影响对评估很重要，因为铁沉积引起的心脏并发症是β-地中海贫血重症患者死亡的主要原因。进一步的研究表明，PCTH具有口服活性，小鼠耐受良好，剂量范围为50至200 mg/kg，每天两次，持续2天。在pcth治疗组中观察到粪铁排泄量呈剂量依赖性增加。200 mg/kg的铁排泄水平与相同剂量的口服有效螯合剂吡哆醛异烟碱酰腙（PIH）和去铁酮（L1）相似。PCTH在肝脏中的有效铁螯合作用是通过其减少铁蛋白- 59fe积累的能力来证明的。50和100 mg/kg/bd剂量的PCTH治疗小鼠3周后，通过体重减轻和一系列生化和血液学指标确定，没有明显的毒性迹象。在超过3周的亚慢性铁排泄研究中，PIH和PCTH （75 mg/kg/bd，连续5天/周）分别使粪便铁排泄量增加到对照的140%和145%。该研究表明，PCTH在100 mg/kg/bd时具有良好的耐受性，并通过口服途径诱导大量铁排泄，这表明其有可能成为替代DFO的候选药物。

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来源期刊

Biochimica et biophysica acta. Molecular basis of disease 生物-生化与分子生物学

CiteScore

12.30

自引率

0.00%

发文量

218

审稿时长

32 days

期刊介绍： BBA Molecular Basis of Disease addresses the biochemistry and molecular genetics of disease processes and models of human disease. This journal covers aspects of aging, cancer, metabolic-, neurological-, and immunological-based disease. Manuscripts focused on using animal models to elucidate biochemical and mechanistic insight in each of these conditions, are particularly encouraged. Manuscripts should emphasize the underlying mechanisms of disease pathways and provide novel contributions to the understanding and/or treatment of these disorders. Highly descriptive and method development submissions may be declined without full review. The submission of uninvited reviews to BBA - Molecular Basis of Disease is strongly discouraged, and any such uninvited review should be accompanied by a coverletter outlining the compelling reasons why the review should be considered.