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Featured researches published by M. Montal.


FEBS Letters | 1993

Design, synthesis and functional characterization of a pentameric channel protein that mimics the presumed pore structure of the nicotinic cholinergic receptor

M. Montal; Takeo Iwamoto; John M. Tomich; Mauricio Montal

Nicotinic cholinergic receptors are membrane proteins composed of five subunits organized around a central aqueous pore. A pentameric channel protein, T5M2δ, that emulates the presumed pore‐forming structure of this receptor was generated by assembling five helix‐forming peptide modules at the lysine ϵ‐amino groups of the 11‐residue template [K∗AK∗KK∗PGK∗EK∗G], where ∗ indicates attachment sites. Helical modules represent the sequence of the M2 segment of the Torpedo californica acetylcholine receptor (AChR) δ subunit; M2 segments are considered involved in pore‐lining. Purified T5M2δ migrates in SDS‐PAGE with an apparent M r~14,000, concordant with a protein of 126 residues. T5M2δ forms cation‐selective channels when reconstituted in planar lipid bilayers. The single channel conductance in symmetric 0.5 M K.C1 is 40 pS. This value approximates the 45 pS single channel conductance characteristic of authentic purified Torpedo AChR, recorded under otherwise identical conditions. These results, together with conformational energy calculations, support the notion that a bundle of five amphipathic a‐helices is a plausible structural motif underlying the inner bundle that forms the pore of the pentameric AChR channel.


Proceedings of the National Academy of Sciences of the United States of America | 1997

Channel formation by antiapoptotic protein Bcl-2

Sharon L. Schendel; Zhihua Xie; M. Montal; Shigemi Matsuyama; Mauricio Montal; John C. Reed


Journal of Biological Chemistry | 1993

Synthetic peptides and four-helix bundle proteins as model systems for the pore-forming structure of channel proteins. II. Transmembrane segment M2 of the brain glycine receptor is a plausible candidate for the pore-lining structure.

G L Reddy; Takeo Iwamoto; John M. Tomich; M. Montal


Journal of Biological Chemistry | 1993

Synthetic peptides and four-helix bundle proteins as model systems for the pore-forming structure of channel proteins. I. Transmembrane segment M2 of the nicotinic cholinergic receptor channel is a key pore-lining structure.

M Oblatt-Montal; L K Bühler; Takeo Iwamoto; John M. Tomich; M. Montal


Nature | 1977

Transmembrane channel formation in rhodopsin-containing bilayer membranes.

M. Montal; Alberto Darszon; H. W. Trissl


Proceedings of the National Academy of Sciences of the United States of America | 1980

Reassembly of protein-lipid complexes into large bilayer vesicles: Perspectives for membrane reconstitution

Alberto Darszon; C. A. Vandenberg; M. Schönfeld; M. H. Ellisman; N. C. Spitzer; M. Montal


Proceedings of the National Academy of Sciences of the United States of America | 1977

Rhodopsin in model membranes: charge displacements in interfacial layers

H. W. Trissl; Alberto Darszon; M. Montal


International Journal of Peptide and Protein Research | 2009

Chemical synthesis and characterization of peptides and oligomeric proteins designed to form transmembrane ion channels

Takeo Iwamoto; Anne Grove; M. Montal; Mauricio Montal; John M. Tomich


Biochemistry | 1979

Rhodopsin--phospholipid complexes in apolar environments: photochemical characterization.

Alberto Darszon; Reto J. Strasser; M. Montal


Journal of Cell Biology | 1979

Incorporation of membrane proteins into large single bilayer vesicles. Application to rhodopsin.

Alberto Darszon; C. A. Vandenberg; M. H. Ellisman; M. Montal

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Alberto Darszon

National Autonomous University of Mexico

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V. Ramakrishnan

Laboratory of Molecular Biology

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Anne Grove

Louisiana State University

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L. Blair

University of California

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M. Philipp

University of California

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Shigemi Matsuyama

Case Western Reserve University

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