Initial Drops in Glomerular Filtration Rate with Certain Drug Classes Retard Kidney Disease Progression

More than 20 years ago, we wrote a review evaluating whether or not angiotensin-converting enzyme inhibitor (ACE)-associated elevations in serum creatinine were of concern after the initiation of these drugs [1]. The beneficial effects of renin-angiotensin system (RAS) blockers, ACE inhibitors, and angiotensin receptor blockers (ARBs) have been known for almost 30 years. These drugs cause an approximate 10–30% initial reduction in estimated glomerular filtration (eGFR) when therapy is initiated [1, 2]. This initial drop in eGFR will vary depending on hydration status and poorly controlled blood pressure duration. It is also well known that these drugs reduce blood pressure and albuminuria and slow the progression of kidney disease in people with and without diabetes [3].

This initial drop in eGFR had been a significant concern for many clinicians and remains so today. In the current issue of the journal, Cherney et al. [4] report the effects of a sodium-glucose cotransporter (SGLT 2) inhibitor on initial changes in estimated glomerular filtration rate (eGFR) and describe that with the initial dip in eGFR, there is an associated improvement in kidney function decay over time (DOI: 10.1159/000524889). These observations are entirely consistent with prior observations with other SGLT 2 inhibitors, ACE inhibitors, and angiotensin receptor blockers (ARBs) as a class [5]. These data add to our understanding that the therapeutic advantage of specific drug classes that ultimately slow diabetic kidney disease progression and reduce cardiovascular (CV) events lowers blood pressure and albuminuria. Still, all have an initially limited decline in eGFR.

In the past 5 years, in addition to the SGLT2 inhibitors [6, 7], an agent from a new class, the nonsteroidal mineralocorticoid receptor antagonists, finerenone, has also been demonstrated to slow the decline in kidney function among those with diabetes, when added to maximally tolerated doses of either ACE inhibitors or ARB [8]. These drug classes also lower blood pressure, reduce albuminuria, and slow the progression of kidney disease, but they are associated with an initial dip in GFR that is somewhat less than that described with ACE inhibitors or ARB [5, 9] Fig. 1. The consistency of the observation that dipping is associated with cardiorenal protection is comforting for clinicians who observe an upward trend in the serum creatinine early in drug initiation.

Fig. 1.

Interaction between cardiorenal protective drugs and eGFR drops.

/WebMaterial/ShowPic/1437494

The actual mechanism of the eGFR dip is not entirely known. Some suspect it may be simply a reduction in glomerular capillary pressure due to a decrease in systemic blood pressure and selective effects on either efferent glomerular arteriolar dilation or some degree of pre-glomerular vasoconstriction, or a combination of the two. There may also be effects on the glomerular ultrafiltration coefficient as well. The magnitude of reduction in eGFR is a function of initial eGFR values; the lower the eGFR, the less the dip [10, 11]. Nonetheless, the consistency of these observations is an important consideration when utilizing these drugs in clinical practice, either alone or in combination with other medications that affect blood pressure or blood volume. Clinicians should be aware that changes in GFR will occur upon the initiation of these drugs.

In clinical practice, clinicians often utilize renal protective drugs with other commonly used antihypertensive drugs such as thiazide and thiazide-like diuretics. These agents facilitate not only better blood pressure reduction but also a further reduction in albuminuria. They can also potentiate the dip observed with renoprotective classes of medications [5]. Many clinicians may stop both diuretics and renal protective drugs because of this initial increase in serum creatinine. However, this is not a wise consideration given that these drugs do have a long-term benefit on kidney function and CV events, and the continuation of these therapies reduces the long-term risk of significant adverse clinical outcomes irrespective of initial changes in serum creatinine. Moreover, a review of older studies, some with as long as a 10-year follow-up, demonstrates the benefits of slowed progression of kidney disease with an initial rise in serum creatinine of up to 30% upon initiation of therapy [12, 13].

Despite the consistency of cardiorenal benefits, many clinicians do not utilize these renal protective drugs or use them in doses not proven to slow kidney disease progression. This is a significant public health concern, and more effort should be provided to educate clinicians that these acute and self-limited changes in kidney function need to be monitored but should not be an indication of a cessation of these cardiorenal protective therapies. With a persistent increase in serum creatinine of 30%, or more, clinicians should be sure that their patients are not taking nonsteroidal anti-inflammatory drugs, are not volume depleted, and rule out clinically significant renal artery stenosis, if necessary, with imaging. The abundance of data supports the continued use of these drugs. It expands the use of these renal protective therapies in clinical practice to take full advantage of their potential for arresting the rate of progression of kidney and cardiovascular disease. This is evident from data on many recent outcome studies [13, 14].

Conflict of Interest Statement

George Bakris: supported by T32 NIH grant DK07011, consultant to Bayer, KBP Biosciences, Ionis, Alnylam, Astra Zeneca, Quantum Genomics, Horizon, Novo Nordisk, Dia Medica Therapeutics, InREGEN. Matthew Weir: supported by R01 DK116095, U01 DK1061022, R01 DK120886, U01 DK129884, and Scientific advisor: AstraZeneca, Bayer, Merck, Boehringer-Ingelheim, Janssen, NovoNordisk, Akebia, Vifor.

Funding Sources

There is no funding involved in this editorial.

Author Contributions

Equal contributions were made by both Dr. G.L. Bakris and Dr. M.R. Weir.

Copyright: All rights reserved. No part of this publication may be translated into other languages, reproduced or utilized in any form or by any means, electronic or mechanical, including photocopying, recording, microcopying, or by any information storage and retrieval system, without permission in writing from the publisher.
Drug Dosage: The authors and the publisher have exerted every effort to ensure that drug selection and dosage set forth in this text are in accord with current recommendations and practice at the time of publication. However, in view of ongoing research, changes in government regulations, and the constant flow of information relating to drug therapy and drug reactions, the reader is urged to check the package insert for each drug for any changes in indications and dosage and for added warnings and precautions. This is particularly important when the recommended agent is a new and/or infrequently employed drug.
Disclaimer: The statements, opinions and data contained in this publication are solely those of the individual authors and contributors and not of the publishers and the editor(s). The appearance of advertisements or/and product references in the publication is not a warranty, endorsement, or approval of the products or services advertised or of their effectiveness, quality or safety. The publisher and the editor(s) disclaim responsibility for any injury to persons or property resulting from any ideas, methods, instructions or products referred to in the content or advertisements.

留言 (0)

沒有登入
gif