Systemic Messenger RNA Therapy as a Treatment for Methylmalonic Acidemia

Ding, An; Schneller, Jessica L.; Frassetto, Andrea; Liang, Shi; Zhu, Xinwen; Park, Ji-Sun; Theisen, Matt; Hong, Sue-Jean; Zhou, Jianchang; Rajendran, Raj; Levy, Becca R.; Howell, Robert D.; Besin, Gilles; Presnyak, Vladimir; Sabnis, Staci; Murphy-Benenato, Kerry E.; Kumarasinghe, E. Sathyajith; Salerno, Timothy; Mihai, Cosmin; Lukacs, C.M.; Chandler, Randy J.; Guey, Lin T.; Venditti, Charles P.; Martini, Paolo G.V.

doi:10.1016/j.celrep.2017.11.081

Cited by 184 publications

(134 citation statements)

References 51 publications

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“…Similar to the Weissman work, Thran and colleagues observed a disproportionate increase of antibody serum titers with elevated mRNA doses. Onset of antibody expression was rather rapid, being already substantial 2 h after injection and reaching peak levels after approximately 4 h. This confirms findings on other mRNA-mediated protein therapies showing that mRNA starts accumulating in hepatocytes within minutes after administration and leads to substantial protein levels within a couple of hours [223,231]. Serum half-life of IgG antibodies appeared to be in the range of 1 week and thus slightly longer compared to Pardi et al [267].…”

Section: Mrna-mediated Antibody Expressionsupporting

confidence: 82%

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mRNA as novel technology for passive immunotherapy

Schlake¹,

Theß²,

Thran³

et al. 2018

Cell. Mol. Life Sci.

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While active immunization elicits a lasting immune response by the body, passive immunotherapy transiently equips the body with exogenously generated immunological effectors in the form of either target-specific antibodies or lymphocytes functionalized with target-specific receptors. In either case, administration or expression of recombinant proteins plays a fundamental role. mRNA prepared by in vitro transcription (IVT) is increasingly appreciated as a drug substance for delivery of recombinant proteins. With its biological role as transient carrier of genetic information translated into protein in the cytoplasm, therapeutic application of mRNA combines several advantages. For example, compared to transfected DNA, mRNA harbors inherent safety features. It is not associated with the risk of inducing genomic changes and potential adverse effects are only temporary due to its transient nature. Compared to the administration of recombinant proteins produced in bioreactors, mRNA allows supplying proteins that are difficult to manufacture and offers extended pharmacokinetics for short-lived proteins. Based on great progress in understanding and manipulating mRNA properties, efficacy data in various models have now demonstrated that IVT mRNA constitutes a potent and flexible platform technology. Starting with an introduction into passive immunotherapy, this review summarizes the current status of IVT mRNA technology and its application to such immunological interventions.

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Section: Mrna-mediated Antibody Expressionsupporting

confidence: 82%

“…However, this can in principle be counteracted by optimization towards better biocompatibility. In case of LNPs, fast degradation was shown to be particularly important [231,232,269].…”

Section: Discussionmentioning

confidence: 99%

mRNA as novel technology for passive immunotherapy

Schlake¹,

Theß²,

Thran³

et al. 2018

Cell. Mol. Life Sci.

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“…An et al demonstrate that for MMA, intravenous administration of mRNA encoding Mut using a biodegradable lipid nanoparticle, results in a 75% reduction of plasma methylmalonic acid and increased MCM activity in the liver of Mut −/− mice, and that repeated dosing led to weight gain and improved survival. To the best of our knowledge, no mRNA treatment for PA has been reported.…”

Section: Therapy Targets and Treatment Strategiesmentioning

confidence: 99%

Pathophysiology of propionic and methylmalonic acidemias. Part 2: Treatment strategies

Haijes

Hasselt

Jans

et al. 2019

J of Inher Metab Disea

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Despite realizing increased survival rates for propionic acidemia (PA) and methylmalonic acidemia (MMA) patients, the current therapeutic regimen is inadequate for preventing or treating the devastating complications that still can occur. The elucidation of pathophysiology of these complications allows us to evaluate and rethink treatment strategies. In this review we display and discuss potential therapy targets and we give a systematic overview on current, experimental and unexplored treatment strategies in order to provide insight in what we have to offer PA and MMA patients, now and in the future. Evidence on the effectiveness of treatment strategies is often scarce, since none were tested in randomized clinical trials. This raises concerns, since even the current consensus on best practice treatment for PA and MMA is not without controversy. To attain substantial improvements in overall outcome, gene, mRNA or enzyme replacement therapy is most promising since permanent reduction of toxic metabolites allows for a less strict therapeutic regime. Hereby, both mitochondrial‐associated and therapy induced complications can theoretically be prevented. However, the road from bench to bedside is long, as it is challenging to design a drug that is delivered to the mitochondria of all tissues that require enzymatic activity, including the brain, without inducing any off‐target effects. To improve survival rate and quality of life of PA and MMA patients, there is a need for systematic (re‐)evaluation of accepted and potential treatment strategies, so that we can better determine who will benefit when and how from which treatment strategy.

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“…These works provided proof-of-concept evidence for the therapeutic value of hepatic MUT activity restoration, as Mut -/- mice were rescued from neonatal mortality and impaired growth in spite of a partial correction of plasma methylmalonic acid levels. With these precedents, the potential of mRNA treatment for MMA has also been recently explored 8. Systemic administration of human MUT (hMUT) mRNA formulated in LNPs as described above demonstrated a rapid (as early as 2 hours after intravenous injection) and sustained expression of hMUT protein in mouse livers (figure 4).…”

Section: Rare Genetic Metabolic Diseases: Difficult To Treat Conditiomentioning

confidence: 99%

“…Systemic administration of human MUT (hMUT) mRNA formulated in LNPs as described above demonstrated a rapid (as early as 2 hours after intravenous injection) and sustained expression of hMUT protein in mouse livers (figure 4). The therapeutic capacity of this hMUT mRNA was tested in two clinically relevant mouse models: Mut -/- mice rescued from perinatal lethality by transgenic expression of MUT in skeletal muscle, and transgenic Mut -/- mice expressing the p.G715V MUT mutant variant found in patients with MMA 8. In the first model, hMUT mRNA administration resulted in a rapid reduction of methylmalonic acid levels in plasma and tissues, including liver, kidney, brain, heart and skeletal muscle.…”

Section: Rare Genetic Metabolic Diseases: Difficult To Treat Conditiomentioning

confidence: 99%

Messenger RNA therapy for rare genetic metabolic diseases

Berraondo

Martini

Avila

et al. 2019

Gut

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Decades of intense research in molecular biology and biochemistry are fructifying in the emergence of therapeutic messenger RNAs (mRNA) as a new class of drugs. Synthetic mRNAs can be sequence optimised to improve translatability into proteins, as well as chemically modified to reduce immunogenicity and increase chemical stability using naturally occurring uridine modifications. These structural improvements, together with the development of safe and efficient vehicles that preserve mRNA integrity in circulation and allow targeted intracellular delivery, have paved the way for mRNA-based therapeutics. Indeed, mRNAs formulated into biodegradable lipid nanoparticles are currently being tested in preclinical and clinical studies for multiple diseases including cancer immunotherapy and vaccination for infectious diseases. An emerging application of mRNAs is the supplementation of proteins that are not expressed or are not functional in a regulated and tissue-specific manner. This so-called ‘protein replacement therapy’ could represent a solution for genetic metabolic diseases currently lacking effective treatments. Here we summarise this new class of drugs and discuss the preclinical evidence supporting the potential of liver-mediated mRNA therapy for three rare genetic conditions: methylmalonic acidaemia, acute intermittent porphyria and ornithine transcarbamylase deficiency.

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Systemic Messenger RNA Therapy as a Treatment for Methylmalonic Acidemia

Cited by 184 publications

References 51 publications

mRNA as novel technology for passive immunotherapy

mRNA as novel technology for passive immunotherapy

Pathophysiology of propionic and methylmalonic acidemias. Part 2: Treatment strategies

Messenger RNA therapy for rare genetic metabolic diseases

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