SGLT2抑制剂和芬烯酮:治疗糖尿病肾病的友好组合?

Adlyne Reena Asirvatham, Arthur Joseph Asirvatham, Shriraam Mahadevan
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摘要

几十年来,实现血糖控制、目标血压和肾素-血管紧张素-醛固酮系统(RAAS)阻断仍然是延缓糖尿病肾病(DKD)进展的治疗干预措施。CREDENCE和DAPA-CKD试验结果显示,当SGLT2抑制剂被推荐用于降低估计肾小球滤过率(eGFR)、终末期肾病(ESRD)和肾性死亡的进行性恶化风险时,DKD的管理发生了重大转变。尽管目前有可用的治疗方法,但心脏死亡、进展为ESRD的风险和肾脏替代治疗的需求仍然很高。Finerenone是一种较新的强效选择性非甾体矿皮质激素受体拮抗剂(MRA),在FIDELIO-DKD和FIGARO-DKD研究中分别显示其可降低原发性复合肾脏和心血管预后。虽然SGLT2抑制剂除了降低肾小球高滤过外,还对细胞和代谢功能有直接影响,但细烯酮主要抑制矿皮质激素通路依赖性炎症和纤维化。dapag列净在DAPA-CKD试验中的肾脏益处与MRA无关,同样,finenone在FIDELIO和FIGARO研究中的益处与SGLT2i无关。此外,同时使用SGLT2抑制剂显著降低了MRA严重高钾血症的风险,使该组合成为更安全的选择。尽管现有数据支持这两种药物在保护肾脏和心脏功能方面可能具有独特和互补的机制,但目前还缺乏推荐在DKD中常规使用SGLT2抑制剂和MRA的有力证据。然而,正在进行的评估恩格列净和芬芬酮双重治疗优势的CONFIDENCE研究结果将值得了解这种友好的双重治疗的益处。
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SGLT2 Inhibitors and Finerenone: A friendly Duo in the Treatment of Diabetic Kidney Disease?

For decades, achieving glycemic control, target blood pressure, and renin-angiotensin-aldosterone system (RAAS) blockade remained to be the therapeutic interventions for retarding diabetic kidney disease (DKD) progression. The management of DKD showed major transformation when SGLT2 inhibitors were recommended to reduce the risk of progressive deterioration in estimated glomerular filtration rate (eGFR), end-stage renal disease (ESRD), and renal death following results of CREDENCE and DAPA-CKD trials. Despite currently available therapeutic approaches, the risk of cardiac death, progression to ESRD, and requirement of renal replacement therapy remains high. Finerenone is the newer potent selective nonsteroidal mineralocorticoid receptor antagonist (MRA) that showed reduction in primary composite renal and CV outcomes in FIDELIO-DKD and FIGARO-DKD studies, respectively. While SGLT2 inhibitors have direct effects on cellular and metabolic functions besides reduction in glomerular hyperfiltration, finerenone primarily inhibits mineralocorticoid pathway-dependent inflammation and fibrosis. The renal benefits of dapagliflozin in the DAPA-CKD trial were regardless of MRA, and likewise, the benefits of finerenone in FIDELIO and FIGARO studies were irrespective of SGLT2i. Moreover, the risk of serious hyperkalemia with MRA was significantly reduced by concomitant use of SGLT2 inhibitors, making this combination a safer choice. Even though available data support the fact that this duo possibly has distinct as well as complementary mechanisms in protecting renal and cardiac functions, strong evidence to recommend routine use of the combination of SGLT2 inhibitors and MRA in DKD is currently lacking. However, the results of the ongoing CONFIDENCE study evaluating superiority of dual therapy of empagliflozin and finerenone will be worthwhile to understand the benefits of this friendly duo.

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