Chemical Modification of Interleukin-10 with Mannose 6-Phosphate Groups Yields a Liver-Selective Cytokine

Rachmawati, Heni; Reker‐Smit, Catharina; Hooge, Marjolijn N. Lub-de; Loenen-Weemaes, Anne-miek van; Poelstra, Klaas; Beljaars, Leonie

doi:10.1124/dmd.106.013490

Cited by 26 publications

(14 citation statements)

References 42 publications

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“…Mannose 6-phosphate (M6P)-modified nanoparticles, such as M6P-HSA (or M6P-HSA-liposome), and N-(2-hydroxypropyl) methacrylamide, which contains M6P and tetrapeptide (GFLG), have been used to target stellate cells (Adrian et al, 2007;Beljaars et al, 2001;Li et al, 2009;van Beuge et al, 2011van Beuge et al, , 2013Yang et al, 2009). However, they are also taken up by Kupffer cells and LSECs because M6P-modified delivery systems can accumulate on the scavenger receptors expressed on these cells (Rachmawati et al, 2007). Administration of polyinosinic acid, an inhibitor of scavenger receptors, was found to inhibit the accumulation of M6P-modified nanoparticles in Kupffer cells and LSECs, but not in stellate cells (Adrian et al, 2007), because stellate cells take up M6P-modified nanoparticles through mannose-6-phosphate/insulin-like growth factor II, receptor-mediated endocytosis (Rachmawati et al, 2007).…”

Section: Use Of Liver Cell-targeted Delivery Systems For Treating Hepmentioning

confidence: 99%

“…However, they are also taken up by Kupffer cells and LSECs because M6P-modified delivery systems can accumulate on the scavenger receptors expressed on these cells (Rachmawati et al, 2007). Administration of polyinosinic acid, an inhibitor of scavenger receptors, was found to inhibit the accumulation of M6P-modified nanoparticles in Kupffer cells and LSECs, but not in stellate cells (Adrian et al, 2007), because stellate cells take up M6P-modified nanoparticles through mannose-6-phosphate/insulin-like growth factor II, receptor-mediated endocytosis (Rachmawati et al, 2007). Interestingly, HSA terminated with 28 M6P [M6P(28)-HSA] strongly binds to activated stellate cells, but not to quiescent stellate cells (Beljaars et al, 2001).…”

Section: Use Of Liver Cell-targeted Delivery Systems For Treating Hepmentioning

confidence: 99%

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Liver cell-targeted delivery of therapeutic molecules

Kang

Toita

Murata

2015

Critical Reviews in Biotechnology

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The liver is the largest internal organ in mammals and is involved in metabolism, detoxification, synthesis of proteins and lipids, secretion of cytokines and growth factors and immune/inflammatory responses. Hepatitis, alcoholic or non-alcoholic liver disease, hepatocellular carcinoma, hepatic veno-occlusive disease, and liver fibrosis and cirrhosis are the most common liver diseases. Safe and efficient delivery of therapeutic molecules (drugs, genes or proteins) into the liver is very important to increase the clinical efficacy of these molecules and to reduce their side effects in other organs. Several liver cell-targeted delivery systems have been developed and tested in vivo or ex vivo/in vitro. In this review, we discuss the literature concerning liver cell-targeted delivery systems, with a particular emphasis on the results of in vivo studies.

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Section: Use Of Liver Cell-targeted Delivery Systems For Treating Hepmentioning

confidence: 99%

Section: Use Of Liver Cell-targeted Delivery Systems For Treating Hepmentioning

confidence: 99%

Liver cell-targeted delivery of therapeutic molecules

Kang

Toita

Murata

2015

Critical Reviews in Biotechnology

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“…Other proposed approaches to target specific tissues are the use of fusion proteins of IL-10 and monoclonal antibodies specific for the targeted cell type, that has been shown to be effective in an experimental model of rheumatoid arthritis [48], and the chemical alteration of IL-10. IL-10 modified with mannose-6 phosphate shows a prevalent homing to the liver, in particular to fibrogenic hepatic stellate cells expressing the mannose 6 phosphate/insulin-like growth factor II receptor, and could be applied to the treatment of cirrhosis [49]. The safety of some of these approaches is still in question, but they hold the promise to allow the targeted deliver of IL-10 into specific tissues or cell types and/or a regulated IL-10 production by the patient, thus reducing the systemic impact of the therapy.…”

Section: Il-10 and Il-10 Agonistsmentioning

confidence: 99%

Caveats Regarding the Use of IL-10 and IL-10 Antagonist as Immunotherapeutic Factors

Colino¹

2007

LDDD

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“…Both in vitro and in vivo studies in male Wistar rats showed that these NPs were a potent nanocarrier for targeting HSC and can utilize the immune response against fibrosis. [63][64][65] A similar kind of study was done by another group using M6P to modify HSA, which showed successful delivery of DOX, cisplatin and chlorambucil for the pharmacotherapy of liver fibrosis. The reduction in liver fibrosis markers was confirmed using in vitro studies as well as in vivo studies in BDL rats.…”

Section: Other Npsmentioning

confidence: 99%

Nanoparticles for the treatment of liver fibrosis

Surendran¹,

Thomas²,

Moon³

et al. 2017

IJN

114

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Chronic liver diseases represent a global health problem due to their high prevalence worldwide and the limited available curative treatment options. They can result from various causes, both infectious and noninfectious diseases. The application of nanoparticle (NP) systems has emerged as a rapidly evolving area of interest for the safe delivery of various drugs and nucleic acids for chronic liver diseases. This review presents the pathogenesis, diagnosis and the emerging nanoparticulate systems used in the treatment of chronic liver diseases caused by liver fibrosis. Activated hepatic stellate cell (HSC) is considered to be the main mechanism for liver fibrosis. Ultrasonography and magnetic resonance imaging techniques are widely used noninvasive diagnostic methods for hepatic fibrosis. A variety of nanoparticulate systems are mainly focused on targeting HSC in the treatment of hepatic fibrosis. As early liver fibrosis is reversible by current NP therapy, it is being studied in preclinical as well as clinical trials. Among various nanoparticulate systems, inorganic NPs, liposomes and nanomicelles have been widely studied due to their distinct properties to deliver drugs as well as other therapeutic moieties. Liposomal NPs in clinical trials is considered to be a milestone in the treatment of hepatic fibrosis. Currently, NP therapy for liver fibrosis is updating fast, and hopefully, it can be the future remedy for liver fibrosis.

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Chemical Modification of Interleukin-10 with Mannose 6-Phosphate Groups Yields a Liver-Selective Cytokine

Cited by 26 publications

References 42 publications

Liver cell-targeted delivery of therapeutic molecules

Liver cell-targeted delivery of therapeutic molecules

Caveats Regarding the Use of IL-10 and IL-10 Antagonist as Immunotherapeutic Factors

Nanoparticles for the treatment of liver fibrosis

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