Specific inhibition of <i>Physarum polycephalum</i> DNA‐polymerase‐α‐primase by poly(<scp>l</scp>‐malate) and related polyanions

Holler, Eggehard; Achhammer, Gunthar; Angerer, Bernhard; Gantz, Bruce J.; Hambach, C.; Reisner, Hermine; Seidel, Bettina; Weber, Cornelia; Windisch, C; Braud, Christian; Guérin, P.; Vert, Michel

doi:10.1111/j.1432-1033.1992.tb16894.x

Cited by 27 publications

(34 citation statements)

References 24 publications

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“…Structurally, poly(α,β-(D,L)-aspartic acid) and poly(α,β-(D,L)-malic acid) are similar except the replacement of the amido group in PAA by the ester group in PMLA. Remarkably, the spatial distances of polymer pendant carboxylates are similar, which was recognized in experiments measuring the inhibition of DNA polymerases by polyanions of variable structures [44]. In this study, a similarity of the distance between the negatively charged carboxylates in PMLA and PAA with phosphate groups in nucleic acids has been noted.…”

Section: Examples Of Covalent Nanodelivery Systems Based On Polymesupporting

confidence: 70%

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Covalent nano delivery systems for selective imaging and treatment of brain tumors

Ljubimova

Sun

Mashouf

et al. 2017

Advanced Drug Delivery Reviews

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Nanomedicine is a rapidly evolving form of therapy that holds a great promise in superior drug delivery efficiency and therapeutic efficacy than conventional cancer treatment. In this review, we attempt to cover the benefits and the limitations of current nanomedicines with special attention to covalent nanoconjugates for imaging and drug delivery in brain. The improvement in brain tumor treatment remains dismal despite decades of efforts in drug development and patient care. One of the major obstacles in brain cancer treatment is the poor drug delivery efficiency owing to the unique blood-brain-barrier (BBB) in the CNS. Although various anti-cancer agents are available to treat tumors outside of the CNS, the majority fails to cross the BBB. In this regard, nanomedicines have increasingly drawn attention due to their multi-functionality and versatility. Nano-drugs can penetrate BBB and other biological barriers, and selectively accumulate in tumor cells, while concurrently decreasing systemic toxicity.

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Section: Examples Of Covalent Nanodelivery Systems Based On Polymesupporting

confidence: 70%

“…Polymalic acid of high molecular weight was discovered by its ability to mimic nucleic acids and competitively inhibit DNA polymerase α of Physarum polycephalum , and, to a lesser extent, the activities of DNA polymerases from other organisms [43, 44] (Fig. 3).…”

Section: Examples Of Covalent Nanodelivery Systems Based On Polymementioning

confidence: 99%

Covalent nano delivery systems for selective imaging and treatment of brain tumors

Ljubimova

Sun

Mashouf

et al. 2017

Advanced Drug Delivery Reviews

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“…Subsequent work showed that the slow addition of histone made it possible to assemble nucleosomes without the histone chaperone at near physiological ionic strength. Under these conditions, however, nucleosome assembly could be stimulated by the addition of other chromatin components (e.g., the linker histone H1 and the non-histone protein HMG [7,8]) and acidic polymers (e.g., acidic polypeptide [9,10], poly (L-malate) [11], and RNA [12]). These studies resulted in the isolation of other histone chaperones with different primary structures and demonstrated that there are various types of histone chaperones [13].…”

Section: Histone Chaperonesmentioning

confidence: 99%

Histone chaperones: 30 years from isolation to elucidation of the mechanisms of nucleosome assembly and disassembly

Eitoku

Sato

Senda

et al. 2007

Cell. Mol. Life Sci.

182

197

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Some three decades have passed since the discovery of nucleosomes in 1974 and the first isolation of a histone chaperone in 1978. While various types of histone chaperones have been isolated and functionally analyzed, the elementary processes of nucleosome assembly and disassembly have been less well characterized. Recently, the tertiary structure of a hetero-trimeric complex composed of the histone chaperone CIA/ASF1 and the histone H3-H4 dimer was determined, and this complex was proposed to be an intermediate in nucleosome assembly and disassembly reactions. In addition, CIA alone was biochemically shown to dissociate the histone (H3-H4)2 tetramer into two histone H3-H4 dimers. This activity suggested that CIA regulates the semi-conservative replication of nucleosomes. Here, we provide an overview of prominent histone chaperones with the goal of elucidating the mechanisms that preserve and modify epigenetic information. We also discuss the reactions involved in nucleosome assembly and disassembly.

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“…for DNA polymerases) and is therefore assumed to be involved in DNA replication. [17] The organisms most efficient in producing β-PMA are the black yeasts Aureobasidium sp. [18] and A. pullulans, [19] from which up to 61 g/l and 9.8 g/l culture medium were isolated, respectively.…”

Section: Introductionmentioning

confidence: 99%

Preparation of Free and of Specifically Protected Oligo[β-Malic Acids] for Enzymatic Degradation Studies

Krell¹,

Seebàch

2000

Eur. J. Org. Chem.

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The polyanionic poly[β-(S)-malic acids] (β-PMA) occur in slime molds (myxomycetes), black yeasts and other fungi and are involved in DNA replication. In order to be able to study the cleavage mechanism of β-PMA hydrolases, we have synthesized cyclic and linear oligomers of malic acid (β-OMA) consisting of up to eight residues. To this end, fragments with three different protecting groups were prepared, with allyl ester groups on the C-terminus, TBDPS groups at the O-terminus, and benzyl ester groups at the side chains (Schemes 2, 3, 7). Selective deprotection and fragment coupling (COCl 2 /C 5 H 5 N/CH 2 Cl 2 /-75°C) gave dimers, tetramers, and

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Specific inhibition of Physarum polycephalum DNA‐polymerase‐α‐primase by poly(l‐malate) and related polyanions

Cited by 27 publications

References 24 publications

Covalent nano delivery systems for selective imaging and treatment of brain tumors

Covalent nano delivery systems for selective imaging and treatment of brain tumors

Histone chaperones: 30 years from isolation to elucidation of the mechanisms of nucleosome assembly and disassembly

Preparation of Free and of Specifically Protected Oligo[β-Malic Acids] for Enzymatic Degradation Studies

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