As we delve deep into countless medical journals to uncover the latest on Integrative Medicine’s approach to kidney health, we are always reminded of the value of your time. Our commitment remains steadfast in curating and succinctly summarizing these vital studies for you. Welcome to the March Research and News.

 

March Research and News

 

Reduced Sodium and DASH Diet Impact on Kidney Function: Insights from the DASH-Sodium Trial

In the DASH-Sodium trial, researchers explored the impact of dietary sodium reduction combined with the Dietary Approaches to Stop Hypertension (DASH) diet on kidney function, specifically the estimated glomerular filtration rate (eGFR) measured by cystatin C.

The controlled feeding study involved adults with elevated or stage 1 hypertension who were randomized to either the DASH diet or a control diet, subsequently consuming varying levels of sodium over three 30-day periods.

The study found that while the DASH diet alone did not significantly affect the eGFR, combining it with a low-sodium intake notably decreased the eGFR.

Specifically, transitioning from a high to a low sodium intake resulted in a significant reduction in eGFR. When adjusted for diastolic blood pressure and urinary potassium excretion, the impact of the low sodium-DASH diet on eGFR was somewhat attenuated.

Why is this important?

This study sheds light on the nuanced effects of diet on kidney function, illustrating that a low-sodium version of the DASH diet can lead to a reduction in eGFR over four weeks.

Understanding these dynamics is crucial for developing dietary recommendations, particularly for individuals at risk of hypertension or chronic kidney disease (CKD).

The findings suggest potential implications for the dietary management of kidney health, emphasizing the need for further research to explore the long-term effects of such dietary interventions on kidney function and the progression to CKD.

Read the study.

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Ionized and Total Magnesium Levels in Chronic Kidney Disease: Outcomes and Associated Factors

In this study, investigators examined the relationship between ionized (iMg) and total magnesium (tMg) levels and their impact on major adverse cardiovascular events (MACE) and mortality in patients with chronic kidney disease (CKD).

The study utilized data from the CKD-REIN cohort, focusing on patients with an eGFR of less than 60 mL/min/1.73m², to explore how these magnesium levels correlate with cardiovascular outcomes and mortality before kidney replacement therapy (KRT).

The analysis revealed a strong correlation between serum levels of iMg and tMg, which were both independently associated with eGFR. Interestingly, while the serum tMg levels were linked to an increased risk of MACE and mortality, especially in the highest and lowest tertiles of tMg concentration, the ionized magnesium levels did not show a significant association with these outcomes.

Patients in the highest tertile of serum tMg faced a greater likelihood of experiencing MACE and mortality compared to those in the middle tertile.

Why is this important?

This study underscores the importance of monitoring magnesium levels in CKD patients, given the potential association of total serum magnesium with major cardiovascular events and mortality.

The findings highlight the need for further research to understand the implications of magnesium homeostasis in CKD and its potential as a biomarker or therapeutic target, especially considering the varied results between total and ionized magnesium.

However, the major problem with this study is that it isolated one electrolyte to see its effects on renal and cardiac outcomes. Magnesium in the body does not work alone, and for this study to be really meaningful, it should include levels of other electrolytes and nutrients that magnesium interacts with.

Read the study.

 

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Plasma Levels of Polyunsaturated Fatty Acids and Adverse Kidney Outcomes

In a comprehensive study, researchers examined the association between plasma polyunsaturated fatty acids (PUFA) levels and kidney outcomes in two distinct cohorts from the UK Biobank Study.

Cohort 1 comprised 78,950 participants without chronic kidney disease (CKD), while Cohort 2 included 7,233 participants with CKD.

The study aimed to investigate the relationship between various plasma PUFA components and the risk of incident CKD in the first cohort and the risk of progressing to kidney failure requiring replacement therapy (KFRT) in the second.

The findings indicated that individuals in Cohort 1 with higher plasma PUFA levels were less likely to develop CKD over a median follow-up of 11.9 years. Specifically, the higher quartiles of PUFA showed a significant inverse association with incident CKD, suggesting a protective effect.

In Cohort 2, although total PUFA levels were not linked to the risk of KFRT, higher levels of docosahexaenoic acid (DHA), a specific omega-3 fatty acid, were associated with a reduced risk of progressing to KFRT.

Why is this important?

This study highlights the potential role of polyunsaturated fatty acids in kidney health, showing that higher plasma levels of PUFA are associated with a reduced risk of developing CKD in individuals without pre-existing kidney disease.

Furthermore, for patients with CKD, elevated levels of the omega-3 fatty acid DHA were linked to a lower risk of requiring kidney failure replacement therapy.

These findings suggest that monitoring and potentially modifying plasma PUFA levels could be an important strategy in preventing CKD progression and improving outcomes for individuals with existing kidney disease.

The study provides valuable insights that could inform dietary recommendations and therapeutic interventions aimed at enhancing kidney health and preventing adverse kidney outcomes.

Read the study.

 

 


Fructose and Kidney Health: Insights and Implications

In this perspective, published ahead of print in the journal CJASN, researchers discussed the role of fructose in kidney health.

Fructose, commonly found in fruits, honey, and especially in sugar-sweetened beverages like soft drinks, has seen a marked increase in consumption over recent decades. This rise is paralleled by the increased use of high fructose corn syrup, primarily in sodas.

Beyond dietary sources, the body can endogenously produce fructose, especially in conditions such as diabetes, high carbohydrate diets, or excessive alcohol intake.

Both experimental and epidemiological evidence underscores the role of high fructose intake in chronic kidney disease (CKD) progression.

Animal studies have shown that a high-fructose diet leads to significant kidney damage, characterized by tubulointerstitial lesions, fibrosis, increased epithelial expression of vimentin, and heightened immune cell infiltration.

Additionally, fructose exposure has been linked to the release of inflammatory cytokines from cultured proximal tubular cells, correlating with clinical data that associate fructose consumption with an increased incidence of CKD.

Furthermore, endogenous fructose metabolism, particularly in the proximal tubule cells of the kidneys, plays a crucial role in progressive kidney damage.

This metabolic pathway is activated under diabetic conditions and other stressors like renal hypoxia or high salt intake, leading to inflammation, oxidative stress, and subsequent kidney injury.

This is evidenced by animal models where diabetic mice deficient in fructokinase, an enzyme critical in fructose metabolism, exhibit significantly less renal damage compared to their wild-type counterparts.

The pathological implications of fructose metabolism extend to acute kidney injury scenarios, such as ischemic AKI (iAKI), where fructokinase inhibition has shown protective effects against renal injury in animal studies.

This has paved the way for potential therapeutic interventions, such as the use of fructokinase inhibitors like luteolin and osthole, which have shown promising results in mitigating kidney damage in various models.

Why is this important?

The link between fructose intake and metabolism and kidney health is a critical area of research, especially considering the rising prevalence of CKD globally. Understanding how fructose contributes to kidney damage not only illuminates a potential dietary risk factor but also opens new avenues for therapeutic strategies targeting fructokinase inhibition.

Such interventions could offer novel approaches to prevent or mitigate kidney damage, particularly in CKD and iAKI contexts, underscoring the importance of dietary interventions and novel targets in preserving kidney health and preventing disease progression.

Further research in this domain could significantly impact public health strategies and clinical practices, emphasizing the importance of dietary choices and potential new treatments in kidney disease management.

The perspective article can be downloaded for free via this link.

 

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Review article of the month

Plant-derived compounds for treating autosomal dominant polycystic kidney disease

Autosomal dominant polycystic kidney disease (ADPKD), the prevailing monogenic hereditary kidney disorder, stands as the fourth primary contributor to end-stage kidney disease on a global scale. Notably, recent advancements have emerged in slowing ADPKD advancement through diverse chemical medications like tolvaptan, rapamycin, and somatostatin.

However, a multitude of plant-derived compounds are found to have the potential to attenuate ADPKD progression. This review article discusses these compounds.

You can download the full PDF here.


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