The tissue viability imaging system—Suitable method for discovering minimal skin changes in occupational screenings? Results of a cross‐sectional field study

Weistenhöfer, Wobbeke; Uter, Wolfgang; Bernet, Franziska; Drexler, Hans

doi:10.1111/srt.12686

Cited by 1 publication

(1 citation statement)

References 47 publications

(137 reference statements)

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“…On the one hand, acquisition through the glass chamber attenuated the TiVi signal by a factor of 30% compared to adjacent skin, yet correcting results to account for the attenuation did not change our findings (data not shown). On the other hand, it seems that TiVi is sensitive to pigmented skin 32 and the results we observed for ASA detection were less satisfactory than in the case of LCSI. Other portable tools may therefore be preferable for future studies provided that they accurately measure microvascular blood flow and incur a reasonable cost.…”

Section: Discussioncontrasting

confidence: 81%

Current-Induced Vasodilation Specifically Detects, and Correlates With the Time Since, Last Aspirin Intake: An Interventional Study of 830 Patients

Ramondou

Hersant

Fouquet

et al. 2020

J Cardiovasc Pharmacol Ther

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Background: Galvanic current-induced vasodilation (CIV) is impaired in patients under low-dose aspirin (ASA; ≤ 500 mg/day), but potential covariates and the impact of the time since the last ASA intake are unknown. Objectives: We used tissue viability imaging (TiVi) in patients at risk of cardiovascular disease and examined its association with self-reported treatments. Patients/Methods: We recorded the age, gender, height, weight, smoking status, and use of 14 different drug categories in 822 patients either with known peripheral artery disease or at risk thereof. The difference between TiVi arbitrary units (TAUs) where stimulation was applied and an adjacent skin area was recorded, as well as the time since the last ASA intake. Step-by-step regression analysis was used to determine the factors that affect CIV amplitude. Results and Conclusions: CIV was 28.2 ± 22.9 vs. 14.6 ± 18.0 TAUs (p < 0.001) in patients treated with ASA (n = 287) and not treated with ASA (n = 535), respectively. The main determinants of CIV amplitude, by order of importance, were: aspirin intake, diabetes mellitus, age, and male sex. In ASA-treated patients, the main determinants were diabetes mellitus, time since the last ASA intake, male gender, and age. Non-invasive determination of the physiological effects of low-dose ASA is feasible in routine clinical practice. It could be a clinical approach to provide objective evidence of ASA intake, and potentially could be used to test adherence to treatment in ASA-treated patients.

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Section: Discussioncontrasting

confidence: 81%