Autacoid 14S,21R-Dihydroxy-Docosahexaenoic Acid Counteracts Diabetic Impairment of Macrophage Prohealing Functions

Tian, Haibin; Lü, Yan; Shah, Sunish; Hong, Song

doi:10.1016/j.ajpath.2011.06.026

Cited by 32 publications

(61 citation statements)

References 48 publications

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“…Diabetic wounds are characterized by prolonged chronic inflammation and M⌽ inflammatory activities after acute inflammation, and by altered generation of cytokines and lipid mediators (38,50), which contributes to the impairment of pro-healing functions carried out by macrophages (M⌽s) (53,70). These features contribute to the lack of healing (38,52,70) and repair of injured peripheral nerves. The latter results in peripheral neuropathy and insensitivity to injury, and ultimately the poor healing of diabetic wounds such as foot ulcers (18).…”

mentioning

confidence: 97%

“…NPD1 promotes resolution of inflammation by regulating leukocyte infiltration, increasing M⌽ phagocytosis and evacuation from inflammation site to lymphatic system after efferocytosis (60). NPD1, resolvin D1 (29,32,68), and 14,21-diHDHAs (33,47,69,70) accelerate wound healing. In addition, NPD1 also increases corneal nerve area and neural cell survival (5,6,11,16).…”

mentioning

confidence: 98%

“…M⌽s also produce growth factors, including hepatocyte growth factor (HGF) (7, 73, 80 -82), pro-resolving, anti-inflammatory lipid mediators (20,39,57,70), and IL-10 (3,24,27,43). M⌽s or monocytes from blood or injury sites convert docosahexaenoic acid (DHA) to pro-resolving lipid mediators such as neuroprotectin/protectin D1 (NPD1/PD1, 10R,17S-dihydroxy-docosa-4Z,7Z,11E,13E,15Z,19Z-hexaenoic acid) (34,49,63,64), maresins (65), and resolvins (64), as well as 14,21-dihydroxyDHAs (47).…”

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confidence: 99%

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Neuroprotectin/protectin D1: endogenous biosynthesis and actions on diabetic macrophages in promoting wound healing and innervation impaired by diabetes

Hong

Tian

Lü

et al. 2014

American Journal of Physiology-Cell Physiology

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Dysfunction of macrophages (MΦs) in diabetic wounds impairs the healing. MΦs produce anti-inflammatory and pro-resolving neuroprotectin/protectin D1 (NPD1/PD1, 10R,17S-dihydroxy-docosa-4Z,7Z,11E,13E,15Z,19Z-hexaenoic acid); however, little is known about endogenous NPD1 biosynthesis by MΦs and the actions of NPD1 on diabetic MΦ functions in diabetic wound healing. We used an excisional skin wound model of diabetic mice, MΦ depletion, MΦs isolated from diabetic mice, and mass spectrometry-based targeted lipidomics to study the time course progression of NPD1 levels in wounds, the roles of MΦs in NPD1 biosynthesis, and NPD1 action on diabetic MΦ inflammatory activities. We also investigated the healing, innervation, chronic inflammation, and oxidative stress in diabetic wounds treated with NPD1 or NPD1-modulated MΦs from diabetic mice. Injury induced endogenous NPD1 biosynthesis in wounds, but diabetes impeded NPD1 formation. NPD1 was mainly produced by MΦs. NPD1 enhanced wound healing and innervation in diabetic mice and promoted MΦs functions that accelerated these processes. The underlying mechanisms for these actions of NPD1 or NPD1-modulated MΦs involved 1) attenuating MΦ inflammatory activities and chronic inflammation and oxidative stress after acute inflammation in diabetic wound, and 2) increasing MΦ production of IL10 and hepatocyte growth factor. Taken together, NPD1 appears to be a MΦs-produced factor that accelerates diabetic wound healing and promotes MΦ pro-healing functions in diabetic wounds. Decreased NPD1 production in diabetic wound is associated with impaired healing. This study identifies a new molecular target that might be useful in development of more effective therapeutics based on NPD1 and syngeneic diabetic MΦs for treatment of diabetic wounds.

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confidence: 98%

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confidence: 99%

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Neuroprotectin/protectin D1: endogenous biosynthesis and actions on diabetic macrophages in promoting wound healing and innervation impaired by diabetes

Hong

Tian

Lü

et al. 2014

American Journal of Physiology-Cell Physiology

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“…ROS generation in macrophages was assessed by using the probe 2,7-dichlorofluorescein diacetate (DCFH-DA, 10 mM; Sigma). After I/R (without H 2 O 2 ) treatment, macrophages were cultured with DCFH-DA in RPMI-1640 for 30 min, and DCFH-DA fluorescence was measured by using an excitation wavelength of 480 nm and an emission wavelength of 535 nm [50]. HGF and IGF-1 in MSC conditioned media (DMEM, under hypoxia condition) were analyzed by ELISA kits obtained from RayBiotech and R&D Systems, respectively.…”

Section: Cytokine and Ros Generation Analysismentioning

confidence: 99%

14S,21R-dihydroxy-docosahexaenoic Acid Treatment Enhances Mesenchymal Stem Cell Amelioration of Renal Ischemia/Reperfusion Injury

Tian

Lü

Shah

et al. 2012

Stem Cells and Development

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“…(5). In order for these macrophages to induce regeneration of the implant, they have to differentiate into a pro-healing state [52,53]. This can be achieved by activation of these macrophages which bind anti-Gal coated !-gal nanoparticles via the Fc/Fc#R interaction (Fig.…”

Section: Incorporation Of !-Gal Nanoparticles Into Decellularized Tismentioning

confidence: 99%

Macrophages Recruitment and Activation by α-gal Nanoparticles Accelerate Regeneration and Can Improve Biomaterials Efficacy in Tissue Engineering

Galili¹

2013

TOTERMJ

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This review describes a novel method for accelerating tissue regeneration by !-gal nanoparticles and proposes methods for !-gal nanoparticles mediated increased efficacy of biomaterials used in tissue engineering. !-Gal nanoparticles present multiple !-gal epitopes (Gal!1-3Gal"1-4GlcNAc-R) that bind the most abundant natural antibody in all humans-the anti-Gal antibody, constituting ~1% of immunoglobulins. Anti-Gal/!-gal nanoparticles interaction generates chemotactic complement cleavage peptides that induce rapid and extensive recruitment of macrophages. The subsequent interaction between the Fc portion of anti-Gal coating !-gal nanoparticles and Fc# receptors on macrophages activates these cells to produce cytokines/growth factors that promote tissue regeneration and recruit stem cells. Intradermal injection of !-gal nanoparticles induces localized extensive recruitment and activation of macrophages. These macrophages disappear within 3 weeks without altering normal skin architecture. Application of !-gal nanoparticles onto wounds of anti-Gal producing animals reduces healing time by 40-70%. !-Gal nanoparticles injected into ischemic myocardium induce extensive recruitment of macrophages that secrete cytokines preserving the structure of the ischemic tissue. These macrophages may recruit progenitor cells and/or stem cells that are guided by myocardial microenvironment and extracellular matrix to differentiate into cardiomyocytes. !-Gal nanoparticles applied to nerve injures will recruit macrophages that can promote angiogenesis required for induction of axonal sprouting and thus may regenerate the severed nerve. In tissue engineering, incorporation of !-gal nanoparticles into decellularized tissue and organ implants may improve in vivo regeneration and restore biological function of implants because of accelerated recruitment of macrophages and stem cells.

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Autacoid 14S,21R-Dihydroxy-Docosahexaenoic Acid Counteracts Diabetic Impairment of Macrophage Prohealing Functions

Cited by 32 publications

References 48 publications

Neuroprotectin/protectin D1: endogenous biosynthesis and actions on diabetic macrophages in promoting wound healing and innervation impaired by diabetes

Neuroprotectin/protectin D1: endogenous biosynthesis and actions on diabetic macrophages in promoting wound healing and innervation impaired by diabetes

14S,21R-dihydroxy-docosahexaenoic Acid Treatment Enhances Mesenchymal Stem Cell Amelioration of Renal Ischemia/Reperfusion Injury

Macrophages Recruitment and Activation by α-gal Nanoparticles Accelerate Regeneration and Can Improve Biomaterials Efficacy in Tissue Engineering

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