Vol 27, No 2 (2023)
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Renal resistive index in hypertensive patients: a one centre study

Hasyim Kasim1, Khadijah Khairunnisa Hasyim1, Andi Makbul Aman1, Dimas Bayu1, Nur Fitriani1
Arterial Hypertension 2023;27(2):107-112.

Abstract

Background: Hypertension (HTN) is a leading cause of kidney dysfunction. Renal resistive index (RRI) was an
index to evaluate arterial compliance and/or resistance, reflecting the reduction of kidney function and microalbuminuria.
We investigated the relationship of RRI in hypertensive patients to detect kidney dysfunction early
detection.

Material and methods: This was a cross-sectional study at Wahidin Sudirohusodo hospital in June–November 2022. All hypertensive patients were evaluated for RRI. RRI was examined with intrarenal doppler ultrasound, and a cutoff ≥ 0.70 were used.

Results: This study included 61 subjects. Thirty-five subjects were female, and 26 subjects were male 90.2% of subjects were below 60 years. Estimated glomerular filtration rate (eGFR) level was 90.29 ± 25.19 in RRI < 0.7 and 64.91 ± 31.79 in RRI ≥ 0.7. Our study found there was a significant difference between anti-hypertensive treatment and eGFR level with the RRI group (p-value < 0.05). There was no significant difference in sex, age, proteinuria, and HTN control status in both RRI groups.

Conclusion: The renal resistive index is a useful marker for early renal dysfunction in hypertensive patients despite normal eGFR.

Original paper

Renal resistive index in hypertensive patients: a one centre study

Hasyim KasimKhadijah Khairunnisa HasyimAndi Makbul AmanDimas Bayuand Nur Fitriani
Department of Internal Medicine, Faculty of Medicine, Hasanuddin University, Tamalanrea, Makassar, Indonesia

Address for correspondence: Hasyim Kasim, Department of Internal Medicine, Faculty of Medicine, Hasanuddin University, Tamalanrea, Makassar, Indonesia; e-mail: hasyimkasim.unhas@gmail.com

This article is available in open access under Creative Common Attribution-Non-Commercial-No Derivatives 4.0 International (CC BY-NC-ND 4.0) license, allowing to download articles and share them with others as long as they credit the authors and the publisher, but without permission to change them in any way or use them commercially

Abstract
Background: Hypertension (HTN) is a leading cause of kidney dysfunction. Renal resistive index (RRI) was an index to evaluate arterial compliance and/or resistance, reflecting the reduction of kidney function and microalbuminuria. We investigated the relationship of RRI in hypertensive patients to detect kidney dysfunction early detection.
Material and methods: This was a cross-sectional study at Wahidin Sudirohusodo hospital in June–November 2022. All hypertensive patients were evaluated for RRI. RRI was examined with intrarenal doppler ultrasound, and a cut-off0.70 were used.
Results: This study included 61 subjects. Thirty-five subjects were female, and 26 subjects were male 90.2% of subjects were below 60 years. Estimated glomerular filtration rate (eGFR) level was 90.29 ± 25.19 in RRI < 0.7 and 64.91 ± 31.79 in RRI0.7. Our study found there was a significant difference between anti-hypertensive treatment and eGFR level with the RRI group (p-value < 0.05). There was no significant difference in sex, age, proteinuria, and HTN control status in both RRI groups.
Conclusion: The renal resistive index is a useful marker for early renal dysfunction in hypertensive patients despite normal eGFR.
Key words: hypertension; renal resistive index (RRI); eGFR level; proteinuria
Arterial Hypertens. 2023, vol. 27, no. 2, pages: 107–112
DOI: 10.5603/AH.a2023.0003

Introduction

Renal resistive index (RRI) is an ultrasonographic Doppler measurement of flow velocities in intraparenchymal renal arteries [1]. It is a non-invasive and repeatable method for assessing arterial compliance and/or resistance. RRI appears to have a significant role in assessing various secondary hypertension (HTN) patients. RRI is related to subclinical indicators of target organ damage and represents renal disease progression beyond albuminuria and creatinine clearance. Also, the RRI can evaluate cardiovascular and renal risk [2]. Several studies indicate that this index reflects systemic hemodynamic and depends on the aortic pulse pressure, which is affected by parameters like age, presence of HTN, or diabetes. In patients with widespread atherosclerosis or reduced vascular compliance, RRI may be increased even with normal kidney function [2]. An elevated RRI (≥ 0.70) is usually associated with impaired renal function, increased proteinuria, and poor prognosis [3]. Evaluation of RRI may also contribute to therapeutic decision-making. Given its straightforward assessment, RRI appears as a simple approach and “multifunctional” instrument that might aid in evaluating renal disease progression. The purpose of this review was to evaluate RRI in hypertensive patients.

Material and methods

Subjects

Sixty-one patients with HTN at Wahidin Sudirohusodo Hospital were chosen as a subject. All patients had signed a consent form and confirmed their voluntary participation in this research study. They were given an explanation regarding the purpose, benefits, and what was done in this study and agreed to participate in this research voluntarily. During the study, they had been given the right to ask questions or ask for clarification from researchers if there were still things that were not clear.

All essential HTN patients were evaluated for renal RI at the initial visit. HTN was defined as systolic blood pressure of 140 mm Hg and/or diastolic blood pressure of 90 mm Hg, measured three times in the sitting position using a brachial sphygmomanometer or therapy with antihypertensive medication. The exclusion criteria were chronic kidney disease with dialysis. The ethics committee of the Faculty of Medicine, Hasanuddin University, authorized the study with ethical number UH22090548. The study was conducted in accordance with the Declaration of Helsinki Ethical Principles and Good Clinical Practices.

Blood and urine collection

Using an automated analyser, haemoglobin, creatinine, sodium, potassium, and chloride were determined. The estimated glomerular filtration rate was computed utilizing the equation of Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI).

Duplex doppler ultrasonography

Doppler ultrasonography was used to investigate renal haemodynamics utilizing an HI VISION Avius (Hitachi Aloka Medical, Tokyo, Japan.) and a 3.5-MHz convex probe fitted with a Doppler system. Doppler flow was measured in the interlobar arteries of both kidneys at three distinct places (superior, middle, and inferior) using colour flow mapping as a reference. Then, peak systolic velocity (PSV) and end-diastolic velocity (EDV) were calculated. The average resistive index (RI) was computed using the following formula:

RI = (PSV – EDV)/PSV [4]

Statistical analysis

Statistical analysis was implemented using the statistical package for social sciences (SPSS) software, version 25.0 for Windows. Data are expressed as mean ± SD or median (interquartile range). Both data and normality were analysed using the Kolmogorov-Smirnov test. The chi-square test was used to evaluate significant differences between variable with normal data distribution. Statistical significance was defined as p-value < 0.05.

Results

This study included 61 patients (Tab. 1 and 2). Thirty-five subjects were female, and 26 subjects were male. 90.2% of subjects were below 60 years. Antihypertensive treatment usage was calcium channel blocker (50.8%), angiotensin receptor blocker (9.8%), angiotensin converting enzyme inhibitor (ACEI) (6.6%), a combination of calcium channel blocker (CCB) and angiotensin receptor blocker (ARB) (27.9%), a combination of CCB and ACEI (3.3%), and three combination drugs (1.6%). Based on the RRI group, 88.5% had the RRI value of < 0.7, and 11.5% had an RRI value of0.7. Based on proteinuria, 42.6% had proteinuria and 57.4% had no proteinuria. Based on hypertensive control, accounted 31.1% of subjects had controlled HTN, and 68.9% of subjects were uncontrolled. In Table 3, the average eGFR RRI < 0.7 is 90.29 ± 25.19 and the average RRI0.7 is 64.91 ± 31.79. With a p-value of 0.030, there was a significant difference between eGFR and RRI. Age, systolic, diastolic, pulse rate, haemoglobin, creatinine, and potassium were not significantly different on the RRI (p-value > 0.05). In the RRI 0.7 group, there were 27 CCB subjects, 6 ARB subjects, 4 ACEI subjects, 14 CCB+ARB subjects, 2 CCB + ACEI subjects, and 1 person receiving a combination of all three medicines. In the RRI > 0.7 group, 4 participants had CCB, 0 had ARB, 0 had ACEI, 3 had CCB + ARB, 0 had CCB + ACEi, and 0 had a combination of all 3 medications. There was a correlation between antihypertensive therapy and RRI (p = 0.04) (Tab. 4).

Table 1. Data descriptive

Minimum

Maximum

Average

SD

Age [years]

32.0

63.0

50.7

8.6

Systolic blood pressure [mm Hg]

110.0

214.0

155.4

21.9

Diastolic blood pressure [mm Hg]

63.0

127.0

89.6

12.2

Heart rate [beat/min]

62.0

121.0

88.1

11.2

Haemoglobin [g/dL]

7.4

16.9

12.8

2.3

Creatinine [mg/dL]

0.4

3.4

0.9

0.5

GFR [mL/min/1.73 m2]

14.8

138.0

87.4

26.9

RRI

0.5

0.8

0.6

0.1

Natrium [mEg/L]

127.0

150.0

139.3

4.2

Potassium [mEg/L]

2.8

5.3

3.9

0.6

Chloride [mEg/L]

96.0

113.0

104.8

4.0

Table 2. Data descriptive

Variable

n

%

Sex

Female

35

57.4

Male

26

42.6

Age

< 60 years

55

90.2

≥ 60 years

6

9.8

Antihypertensive treatment

CCB

31

50.8

ARB

6

9.8

ACEI

4

6.6

CCB + ARB

17

27.9

CCB + ACEI

2

3.3

Combination of three

1

1.6

RRI

< 0.7

54

88.5

≥ 0.7

7

11.5

Proteinuria

Normal

35

57.4

Proteinuria

26

42.6

Hypertensive control

Controlled

19

31.1

Uncontrolled

42

68.9

Table 3. Renal resistive index (RRI) profile in hypertensive patient

Variable

RRI

p-value*

< 0.7 (n = 54)

≥ 0.7 (n = 7)

Age

50.0 ± 8.8

55.5 ± 4.1

0.10

Systolic

156.1 ± 21.3

150.1 ± 27.2

0.50

Diastolic

90.5 ± 12.3

83.1 ± 9.9

0.14

Heart rate

88.8 ± 11.3

83.1 ± 9.5

0.21

Haemoglobin

12.7 ± 2.2

13.3 ± 3.1

0.51

Creatinine

0.9 ± 0.3

1.4 ± 0.9

0.10**

eGFR

90.3 ± 25.2

64.9 ± 31.8

0.03**

Potassium

3.9 ± 0.5

4.2 ± 0.5

0.19

Table 4. Relationship of renal resistive index (RRI) and independent variable

Variable

RRI (n,%)

p-value*

< 0,7 (n = 54)

≥ 0,7 (n = 7)

Sex

Female

32 (91.4)

3 (8.6)

0.41

Male

22 (84.0)

4 (15.4)

Age

< 60 years

49 (89.1)

6 (10.9)

0.67

≥ 60 years

5 (83.3)

1 (16.7)

Anti-hypertensive treatment

CCB

27 (87.1)

4 (12.9)

ARB

6 (100.0)

0 (0)

0.04

ACEI

4 (100.0)

0 (0)

CCB + ARB

14 (82.4)

3 (17.6)

CCB + ACEI

2 (100.0)

0 (0)

Combination of three

1 (100.0)

0 (0)

Proteinuria

Normal

29 (82.9)

6 (17.1)

0.10

Proteinuria

25 (96.2)

1 (3.8)

Hypertensive control

Controlled

16 (84.2)

3 (15.8)

0.47

Uncontrolled

38 (90.5)

4 (9.5)

Value (average ± SD)

Creatinine

0.88 ± 0.32

1.37 ± 0.93

0.10**

GFR

90.29 ± 25.19

64.91 ± 31.79

0.03**

Discussion

This study showed a significant relationship between RRI values and eGFR even though the average eGFR value was more than 60 mL/min/1.73 m2. Renal vasodilating capacity was reduced before the onset of established renal damage and in normal RRI values, meaning that functional rather than structural alterations might already be present, indicating a subclinical stage of renal damage. In predicting Chronic Kidney Disease (CKD) progression and poor outcomes in cases with mild to moderate renal impairment, RRI was superior to renal function assessment alone [5]. Four RRI has been linked to a quicker loss in renal function in individuals with proteinuria CKD or diabetics with microalbuminuria, even when GFR levels are normal [6]. In Table 3, there was a significant relationship between RRI and eGFR in 61 hypertensive patients. It seems that lower eGFR values were associated with higher RRI values. A similar relationship was reported by Gaurav et al. who reported that there was a significant negative correlation between RRI and eGFR [7].

This study did not show a significant association with proteinuria. It could be due to the fact that this study did not assess microalbuminuria or proteinuria in 24 hours. Hashimoto et al. studied 133 HTN individuals and found that each 0.1 increase in RRI was related to a 5.4-fold increase in the incidence of albuminuria [8]. In an investigation involving 66 patients with critical HTN, a strong correlation was seen between high RRI and future increases in urine albumin excretion [9].

The only variable that substantially predicted an >50% rise in the urine albumin to creatinine ratio over two years was RRI. The ideal RRI cut-off value that predicted this increase was 0.71 (sensitivity 52.4% and specificity 84.0%). This cut-off value was consistent with other studies indicating that RRI values >0.7 are more prevalent in patients with left ventricular hypertrophy or advanced carotid atherosclerosis and are associated with higher mortality in hypertensive patients with CKD and no clinically significant renal artery stenosis [10, 11].

The assessment of RRI may have therapeutic consequences as well. Our study found there was a significant difference (p < 0.05) between RRI and antihypertensive treatment. During chronic antihypertensive medication, there was evidence that changes in RRI parallel changes in urine albumin excretion [11]. In addition, an increase in RRI indicated intrarenal stiffness and urges care in titrating renin-angiotensin system inhibitors to prevent renal function decline, particularly in CKD patients, diabetics, and the elderly. In particular, Renin angiotensin system inhibitors (RASI) such as valsartan and lisinopril can improve renal function in individuals with essential HTN, particularly those with microalbuminuria, by decreasing renal vascular resistance and so avoiding eventual renal failure [12, 12].

Details on the effect of treatment and RRI are given in Table 5. Overall, the majority of patients have RRI of less than 0.7. RRI values were affected by the type of therapy received by either the controlled or uncontrolled HTN. While monotherapy therapy is effective for controlled and uncontrolled HTN, combined therapy is less effective for uncontrolled therapy. Despite the treatment, none showed statistically significant (p< 0.05).

Table 5. Renal resistive index (RRI) values for controlled and uncontrolled hypertension patients

Hypertension

RRI

Total

p-value

< 0.7

≥ 0.7

Controlled hypertension

Monotherapy

N

12

3

15

0.52

%

80.0%

20.0%

100.0%

Combination therapy

N

7

0

7

%

100.0%

0%

100.0%

Total

N

19

3

22

%

86.4%

13.6%

100.0%

Uncontrolled hypertension

Monotherapy

N

26

1

27

0.08

%

96.3%

3.7%

100.0%

Combination therapy

N

9

3

12

%

75.0%

25.0%

100.0%

Total

N

35

4

39

%

89.7%

10.3%

100.0%

Conclusion

RRI is a useful marker for renal dysfunction in hypertensive patients.

Authorship

H.K.: conceptualization, data collection, writing, funding acquisition. K.K.H.: data collection, methodology. A.M.A.: methodology, writing. D.B.: data modelling. N.F.: writing review and editing.

Conflict of interest

The authors declare no conflict of interest.

Funding

We want to thank the Hasanuddin University, Indonesia for their research grand number 1148/UN4.22/PT.01.06/2022.

Acknowledgments

We would like to thank the Department of Internal Medicine, Wahidin Sudirohusodo Hospital, Makassar, Indonesia for their support.

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