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New Strategies for Anaemia Management in Chronic Kidney Disease

机译:慢性肾病中贫血管理的新策略

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Erythropoiesis-stimulating agents (ESAs) and iron therapy are the standard of care for normocytic normochromic anaemia, which is a frequent comorbidity of patients with chronic kidney disease. In a large percentage of patients, ESAs and iron increase haemoglobin levels, thus reducing the risk of blood transfusions and improving patient quality of life. However, randomised trials have raised some concerns about higher haemoglobin targets and/or high ESA dose use. These concerns include higher cardiovascular and thrombosis risk, cancer progression, and increased mortality. A more cautious approach was then advised and partial anaemia correction (haemoglobin 10-12 g/dl) is now strongly suggested. The clinical concerns about ESAs and economic constraints have led to larger intravenous iron use. However, severe anaphylactic reactions, although infrequent, can occur and excessive iron use may be dangerous as well, possibly causing iron overload. Several attempts are being made to develop new drugs with theoretically better activity and safety, and/or easier manufacturing processes as compared to available ESAs. These include drugs manipulating the hypoxia-inducible transcription factor (HIF) system, which stimulates the endogenous erythro-poietin (EPO) production and avoids unphysiological EPO plasma levels. Several phase I and II studies support the beneficial role of augmenting HIFs to stimulate eryth-ropoiesis. Here we give an update on this new investiga-tional strategy.
机译:促红细胞血液刺激剂(ESAs)和铁疗是常规肾性肾上腺素贫血的护理标准,这是慢性肾疾病患者的常意合并症。在大量的患者中,ESA和铁增加了血红蛋白水平,从而降低了输血的风险,提高了患者的生活质量。然而,随机试验提出了对血红蛋白靶标和/或高ESA剂量使用的一些担忧。这些问题包括更高的心血管和血栓形成风险,癌症进展和增加的死亡率。然后建议更谨慎的方法,并强烈建议偏贫血校正(血红蛋白10-12g / dl)。对ESA和经济限制的临床担忧导致静脉注射较大的铁。然而,严重的过载性和过度的铁使用可能导致铁过载,严重过度的过敏反应虽然可能发生严重的过敏反应。与可用ESA相比,正在通过理论上更好的活动和安全性和/或更容易的制造过程来制作几次尝试。这些包括操纵缺氧诱导型转录因子(HIF)系统的药物,该系统刺激内源性红细胞生物素(EPO)生产,避免了无生物学的EPO血浆水平。几届I和II研究支持增强HIF刺激eryth-ropoiesis的有益作用。在这里,我们有关这一新的Investiga-Tional策略的更新。

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