In recent decades, electrochemical detection of arsenic(III) has been undergoing revolutionary developments with higher sensitivity and lower detection limit. Despite great success, electrochemical detection of As(III) still depends heavily on noble metals (predominantly Au) in a strong acid condition, thus increasing the cost and hampering the widespread application. Here, we report a disposable platform completely free from noble metals for electrochemical detection of As(III) in drinking water under nearly neutral condition by square wave anodic stripping voltammetry. By combining the high adsorptivity of Fe3O4 microspheres toward As(III) and the advantages of room temperature ionic liquid (RTIL), the Fe3O4-RTIL composite modified screen-printed carbon electrode (SPCE) showed even better electrochemical performance than commonly used noble metals. Several ionic liquids with different viscosities and surface tensions were found to have a different effect on the voltammetric behavior toward As(III). Under the optimized conditions, the Fe3O4-RTIL composites offered direct detection of As(III) within the desirable range (10 ppb) in drinking water as specified by the World Health Organization (WHO), with a detection limit (3σ method) of 8 × 10(-4) ppb. The obtained sensitivity was 4.91 μA ppb(-1), which is the highest as far as we know. In addition, a possible mechanism for As(III) preconcentration based on adsorption has been proposed and supported by designed experiments. Finally, this platform was successfully applied to analyzing a real sample collected from Inner Mongolia, China.
Angiotensin II has been shown to be a potent agent in the acceleration of wound repair. Angiotensin (1-7), a fragment of angiotensin II that is not hypertensive, was found to be comparable to angiotensin II in accelerating dermal healing. This activity was evaluated in four models: rat and diabetic mouse full-thickness excisional wounds; rat random flap; and guinea pig partial thickness thermal injury. In all models, angiotensin (1-7) was comparable to angiotensin II. Angiotensin (1-7) accelerated the closure of wounds in diabetic mice and rats. In diabetic mice the resultant tissue at day 25 after injury was more comparable to normal tissue than the fibrotic scar observed in placebo-treated wounds. In the random flap model, angiotensin (1-7) was comparable to angiotensin II in maintaining flap viability (approximately 82%) and flap survival (40%). Finally, angiotensin (1-7) increased proliferation in the hair follicles at the edge of the wound and site of thermal injury, and the number of patent blood vessels on day 7 after partial thickness thermal injury. These data may be partially explained by the effect of angiotensin II and angiotensin (1-7) on keratinocyte proliferation. While platelet-derived growth factor had no effect on keratinocyte proliferation, angiotensin II and angiotensin (1-7) significantly increased keratinocyte proliferation. These data show that angiotensin(1-7) is comparable to angiotensin II in accelerating skin repair. Furthermore, the hypertensive and wound healing effects can be separated within the family of angiotensin peptides.
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