Formation of Stable Vesicles from<i>N</i>- or 3-Alkylindoles:  Possible Evidence for Tryptophan as a Membrane Anchor in Proteins

Abel, Ernesto; Wall, Stephen L. De; Edwards, Wilson B.; Lalitha, S.; Covey, and Douglas F.; Gokel, George W.

doi:10.1021/jo000040l

Cited by 35 publications

(26 citation statements)

References 57 publications

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“…A key factor is probably the steric encumbrance of the side chain, since Trp is believed to be a very good anchor point in the membrane. 20,21 In an attempt to improve the potency of DS1(1-15)-NH 2 we added a Lys residue to the N-terminus. Recent findings indicated that acylation of dermaseptin S4 fragments with long chain fatty acids, with or without an amino function in their structures, is well tolerated in terms of antimicrobial activity and is instrumental in modulating the potency and spectrum of activity in different assay conditions.…”

Section: Resultsmentioning

confidence: 99%

Synthesis and antimicrobial activity of dermaseptin S1 analogues

Savoia

Guerrini

Marzola

et al. 2008

Bioorganic & Medicinal Chemistry

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a b s t r a c tDermaseptins are peptides found in the skin secretions of Phyllomedusinae frogs. These peptides exert lytic action on some microorganisms without substantial haemolysis. In an attempt to understand the antimicrobial activity of these peptides we designed several dermaseptin S1 (ALWKTMLKKLGTMALHAG-KAALGAAADTISQGTQ) (DS1) analogues. All peptides were tested on the growth of prokaryotic (Grampositive and Gram-negative bacteria) and eukaryotic (the yeast Candida albicans and the protozoon Leishmania major) organisms. Our data showed a dose-dependent killing effect by most DS1 derivatives. Maximal antibacterial activity was displayed by a 16-mer peptide that was more active than native DS1.

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Section: Resultsmentioning

confidence: 99%

Synthesis and antimicrobial activity of dermaseptin S1 analogues

Savoia

Guerrini

Marzola

et al. 2008

Bioorganic & Medicinal Chemistry

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“…Therefore, substitution of tryptophan may severely affect the insertion capacity of TM peptides. In many TM domains, including the active domain of the TAP inhibitor ICP47, tryptophan residues are located at the interfacial region, where they serve as a membrane anchor (40,(44)(45)(46)(47).…”

Section: The Journal Of Immunologymentioning

confidence: 99%

Cowpox Virus Protein CPXV012 Eludes CTLs by Blocking ATP Binding to TAP

Luteijn

Hoelen

Kruse

et al. 2014

The Journal of Immunology

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CD8+ CTLs detect virus-infected cells through recognition of virus-derived peptides presented at the cell surface by MHC class I molecules. The cowpox virus protein CPXV012 deprives the endoplasmic reticulum (ER) lumen of peptides for loading onto newly synthesized MHC class I molecules by inhibiting the transporter associated with Ag processing (TAP). This evasion strategy allows the virus to avoid detection by the immune system. In this article, we show that CPXV012, a 9-kDa type II transmembrane protein, prevents peptide transport by inhibiting ATP binding to TAP. We identified a segment within the ER-luminal domain of CPXV012 that imposes the block in peptide transport by TAP. Biophysical studies show that this domain has a strong affinity for phospholipids that are also abundant in the ER membrane. We discuss these findings in an evolutionary context and show that a frameshift deletion in the CPXV012 gene in an ancestral cowpox virus created the current form of CPXV012 that is capable of inhibiting TAP. In conclusion, our findings indicate that the ER-luminal domain of CPXV012 inserts into the ER membrane, where it interacts with TAP. CPXV012 presumably induces a conformational arrest that precludes ATP binding to TAP and, thus, activity of TAP, thereby preventing the presentation of viral peptides to CTLs.

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“…An examination of the KcsA voltage gated potassium channel from Streptomyces lividans suggests that the indole residues of all the tryptophans in the structure occur at the insulator-midpolar boundary [45]. Tryptophan is the rarest of the 20 common amino acids and appears to play an important role as a stabilizing element [46][47][48] (Fig. 6).…”

Section: Design Criteria For Hydraphilesmentioning

confidence: 99%

Coordination and transport of alkali metal cations through phospholipid bilayer membranes by hydraphile channels

Gokel

Daschbach

2008

Coordination Chemistry Reviews

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Hydraphiles are synthetic ionophores that were designed to mimic some properties of protein channels that conduct such cations as sodium. They use macrocyclic (crown) polyethers as amphiphilic headgroups and as entry and exit portals. Their overall length is controlled by covalent links between the two headgroups (distal macrocycles) and the "central relay" unit, typically also an azacrown. The hydraphiles insert in the bilayer membranes of synthetic phospholipid vesicles or vital cells and mediate the transport of cations. The hydraphiles were intended to be models but they are functional channels. Because they are symmetric, they are non-rectifying but they show open-close behavior characteristic of natural channels. Because they are non-rectifying, when they insert into a microbial membrane, they lead to a rapid change in osmotic balance that proves fatal to bacteria.

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Formation of Stable Vesicles fromN- or 3-Alkylindoles: Possible Evidence for Tryptophan as a Membrane Anchor in Proteins

Cited by 35 publications

References 57 publications

Synthesis and antimicrobial activity of dermaseptin S1 analogues

Synthesis and antimicrobial activity of dermaseptin S1 analogues

Cowpox Virus Protein CPXV012 Eludes CTLs by Blocking ATP Binding to TAP

Coordination and transport of alkali metal cations through phospholipid bilayer membranes by hydraphile channels

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