6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES

Objectives: It is widely thought that excess pulsatile pressure energy from increased stiffness of large central arteries (macro-vasculature) is transmitted to capillary networks (micro-vasculature) and causes end-organ damage (i.e. kidneys). However, this hypothesis has never been tested, and we so...

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Main Authors: Rachel Climie, Dean Picone, Sarah Blackwood, Ahmad Qasem, Stephen Rattigan, James Sharman
Format: Article
Language:English
Published: Atlantis Press 2016-11-01
Series:Artery Research
Online Access:https://www.atlantis-press.com/article/125930424/view
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spelling doaj-275f523671ea4dd7b8f4c966cf8662da2020-11-25T03:37:40ZengAtlantis PressArtery Research 1876-44012016-11-011610.1016/j.artres.2016.10.0436.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETESRachel ClimieDean PiconeSarah BlackwoodAhmad QasemStephen RattiganJames SharmanObjectives: It is widely thought that excess pulsatile pressure energy from increased stiffness of large central arteries (macro-vasculature) is transmitted to capillary networks (micro-vasculature) and causes end-organ damage (i.e. kidneys). However, this hypothesis has never been tested, and we sought to achieve this by examining people with increased macro-vascular stiffness (patients with type 2 diabetes T2DM) compared with non-diabetic controls. Methods: Among 13 T2DM (68±6 years) and 15 controls (58±11 years) macro-vascular function was measured by aortic stiffness and radial artery waveforms by tonometry. Forearm micro-vascular waveforms were simultaneously measured via low power laser Doppler flowmetry, with augmentation index (AIx) and augmented pressure (AP) derived on all waveforms. Kidney function was assessed by estimated glomerular filtration rate (eGFR). Results: Aortic stiffness was higher among T2DM (9.3±2.5 vs 7.5±1.4 m/s, p=0.046). There was an obvious pulsatile micro-vascular waveform, with qualitative features similar to radial waveforms. Macro-vasculature AIx and AP were significantly related to micro-vasculature AIx (r=0.428. p=0.005 and r=0.545, p=0.004 respectively). Micro-vascular (but not macro-vascular) AIx was associated with eGFR in T2DM (r=−0.632, p=0.037). Conclusions: This is the first in-human evidence of pulsatile pressure interaction between the macro-vasculature and micro-vasculature, and provides potential explanation for accelerated kidney dysfunction.https://www.atlantis-press.com/article/125930424/view
collection DOAJ
language English
format Article
sources DOAJ
author Rachel Climie
Dean Picone
Sarah Blackwood
Ahmad Qasem
Stephen Rattigan
James Sharman
spellingShingle Rachel Climie
Dean Picone
Sarah Blackwood
Ahmad Qasem
Stephen Rattigan
James Sharman
6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES
Artery Research
author_facet Rachel Climie
Dean Picone
Sarah Blackwood
Ahmad Qasem
Stephen Rattigan
James Sharman
author_sort Rachel Climie
title 6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES
title_short 6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES
title_full 6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES
title_fullStr 6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES
title_full_unstemmed 6.7 FIRST EVIDENCE OF PULSATILE PRESSURE INTERACTION BETWEEN THE MACRO-VASCULATURE AND MICRO-VASCULATURE: PROOF-OF-CONCEPT BY ASSOCIATION WITH KIDNEY DYSFUNCTION AMONG PATIENTS WITH TYPE 2 DIABETES
title_sort 6.7 first evidence of pulsatile pressure interaction between the macro-vasculature and micro-vasculature: proof-of-concept by association with kidney dysfunction among patients with type 2 diabetes
publisher Atlantis Press
series Artery Research
issn 1876-4401
publishDate 2016-11-01
description Objectives: It is widely thought that excess pulsatile pressure energy from increased stiffness of large central arteries (macro-vasculature) is transmitted to capillary networks (micro-vasculature) and causes end-organ damage (i.e. kidneys). However, this hypothesis has never been tested, and we sought to achieve this by examining people with increased macro-vascular stiffness (patients with type 2 diabetes T2DM) compared with non-diabetic controls. Methods: Among 13 T2DM (68±6 years) and 15 controls (58±11 years) macro-vascular function was measured by aortic stiffness and radial artery waveforms by tonometry. Forearm micro-vascular waveforms were simultaneously measured via low power laser Doppler flowmetry, with augmentation index (AIx) and augmented pressure (AP) derived on all waveforms. Kidney function was assessed by estimated glomerular filtration rate (eGFR). Results: Aortic stiffness was higher among T2DM (9.3±2.5 vs 7.5±1.4 m/s, p=0.046). There was an obvious pulsatile micro-vascular waveform, with qualitative features similar to radial waveforms. Macro-vasculature AIx and AP were significantly related to micro-vasculature AIx (r=0.428. p=0.005 and r=0.545, p=0.004 respectively). Micro-vascular (but not macro-vascular) AIx was associated with eGFR in T2DM (r=−0.632, p=0.037). Conclusions: This is the first in-human evidence of pulsatile pressure interaction between the macro-vasculature and micro-vasculature, and provides potential explanation for accelerated kidney dysfunction.
url https://www.atlantis-press.com/article/125930424/view
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