First-in-human use of a marine oxygen carrier (M101) for organ preservation: A safety and proof-of-principle study

Meur, Yann Le; Badet, Lionel; Essig, Marie; Thierry, Antoine; Büchler, Matthias; Drouin, S.; Deruelle, C.; Morélon, Emmanuel; Pesteil, Francis; Delpech, P.; Boutin, Jean-Michel; Renard, Félix; Barrou, B.

doi:10.1111/ajt.15798

Cited by 47 publications

(56 citation statements)

References 31 publications

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“…However, in the field of kidney transplantation, a medico-economic study (called OXYOP2) is currently comparing the costs of kidney transplantation depending on whether the graft is HOPE or SCS+M101 preserved. This study is the continuation of the OXYOP trial, 17 which showed that the rate of patients necessitating at least one post-transplant dialysis was significantly lower in SCS+M101preserved kidneys compared with HOPE-preserved kidneys (7% vs. 26%, p = 0.038). As a comparison to this 19% difference in delayed graft function (DGF) rates, an international randomised, controlled trial, comparing HOPE or SCS in deceased-donor kidney transplantation 29 reported DGF rates of 20.8% and 26.5% in SCS and HOPE groups, respectively.…”

Section: Discussionmentioning

confidence: 85%

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Adding the oxygen carrier M101 to a cold-storage solution could be an alternative to HOPE for liver graft preservation

et al. 2020

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Background & Aims: Hypothermic oxygenated machine perfusion (HOPE) is a promising technique for providing oxygen to the liver during graft preservation; however, because of associated logistical constraints, addition of an oxygen transporter to static cold-storage solutions (SCS) might be easier. M101 is marine worm haemoglobin that has been shown to improve kidney preservation in the clinic when added to SCS. This study evaluated the effects of the addition of M101 to SCS on the quality of pig liver graft preservation. Methods: Pig liver grafts were preserved using SCS, HOPE, or SCS+M101, and the liver functions were compared during cold preservation and after orthotopic allotransplantation (OLT) in pigs. Results: During preservation of the liver grafts, mitochondrial function, ATP synthesis, antioxidant capacities, and hepatocyte architecture were better preserved, and free radical production, antioxidant activities, and inflammatory mediators were lower, with HOPE or SCS+M101 than with SCS alone. However, after 1 h of preservation, liver functions with HOPE were superior to those with SCS+M101. After 6 h of preservation and OLT, blood levels of aspartate and alanine aminotransferases and lactate dehydrogenase increased with a peak effect at Day 1 post-transplant; values were similar with HOPE and SCS+M101, and were significantly lower than those in the SCS group. At Days 1 and 3, tumor necrosis factor a levels remained lower with HOPE and SCS+M101 vs. SCS. At Day 7, liver cell necrosis and inflammation were less marked in both oxygenated groups. Conclusions: When added to SCS, M101 effectively oxygenates liver grafts during preservation, preventing post-transplant injury; although graft performances are below those achieved with HOPE.

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Section: Discussionmentioning

confidence: 85%

“…[13][14][15][16] Recently, in a French clinical trial using kidney transplantation from deceased donors, M101 demonstrated safety and efficacy, drastically decreasing the rate of delayed graft function recovery from 26% to 7%. 17 However, M101 performance in cold-stored liver graft remains to be studied.…”

Section: Introductionmentioning

confidence: 99%

Adding the oxygen carrier M101 to a cold-storage solution could be an alternative to HOPE for liver graft preservation

et al. 2020

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“…Interestingly, first M101 use in human clinical trial demonstrated that kidney preservation with M101 solution (1 g/L) before transplantation, improved graft survival and renal function. No immunological/ allergic reactions or infections were reported confirming its absence of cytotoxicity and immunogenicity 38 . This study establishes the cytocompatibility of M101 (1 g/L) in EC as they represent the first line of defense in the periodontium against any foreign aggression 12 .…”

Section: Discussionmentioning

confidence: 90%

“…S1-S3). The selected concentration used in this study (1 g/L) has already demonstrated positive outcomes in vivo and in clinical trials 33,38 .…”

Section: Discussionmentioning

confidence: 99%

A therapeutic oxygen carrier isolated from Arenicola marina decreased P. gingivalis induced inflammation and tissue destruction

Batool

Stutz

Petit

et al. 2020

Sci Rep

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The control of inflammation and infection is crucial for periodontal wound healing and regeneration. M101, an oxygen carrier derived from Arenicola marina, was tested for its anti-inflammatory and anti-infectious potential based on its anti-oxidative and tissue oxygenation properties. In vitro, no cytotoxicity was observed in oral epithelial cells (EC) treated with M101. M101 (1 g/L) reduced significantly the gene expression of pro-inflammatory markers such as TNF-α, NF-κΒ and RANKL in P. gingivalis-LPS stimulated and P. gingivalis-infected EC. The proteome array revealed significant down-regulation of pro-inflammatory cytokines (IL-1β and IL-8) and chemokine ligands (RANTES and IP-10), and upregulation of pro-healing mediators (PDGF-BB, TGF-β1, IL-10, IL-2, IL-4, IL-11 and IL-15) and, extracellular and immune modulators (TIMP-2, M-CSF and ICAM-1). M101 significantly increased the gene expression of Resolvin-E1 receptor. Furthermore, M101 treatment reduced P. gingivalis biofilm growth over glass surface, observed with live/dead analysis and by decreased P. gingivalis 16 s rRNA expression (51.7%) (p < 0.05). In mice, M101 reduced the clinical abscess size (50.2%) in P. gingivalis-induced calvarial lesion concomitant with a decreased inflammatory score evaluated through histomorphometric analysis, thus, improving soft tissue and bone healing response. Therefore, M101 may be a novel therapeutic agent that could be beneficial in the management of P. gingivalis associated diseases.

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“…This molecule has been administered on human for transplantation as an additive in conservative solution [9] , but never directly intravenously (IV), this study revealed the safety of this product considered as a medical device of class III. However, several published preclinical data showed an effective way to transfer oxygen to hypoxia, in particular to the brain, in a study published in the journal of Neurotrauma by the Naval Medical Research Centers on Trauma brain injury animal model.…”

Section: The Hypothesismentioning

confidence: 89%

Combating hypoxemia in COVID-19 patients with a natural oxygen carrier, HEMO2Life® (M101)

Lupon

Lellouch

Zal³

et al. 2021

Medical Hypotheses

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First-in-human use of a marine oxygen carrier (M101) for organ preservation: A safety and proof-of-principle study

Cited by 47 publications

References 31 publications

Adding the oxygen carrier M101 to a cold-storage solution could be an alternative to HOPE for liver graft preservation

Adding the oxygen carrier M101 to a cold-storage solution could be an alternative to HOPE for liver graft preservation

A therapeutic oxygen carrier isolated from Arenicola marina decreased P. gingivalis induced inflammation and tissue destruction

Combating hypoxemia in COVID-19 patients with a natural oxygen carrier, HEMO2Life® (M101)

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