Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major

Tracy Arakaki; Isolde Le Trong; Eric Phizicky; Erin Quartley; George DeTitta; Joseph Luft; Angela Lauricella; Lori Anderson; Oleksandr Kalyuzhniy; Elizabeth Worthey; Peter J. Myler; David Kim; David Baker; Wim G.J. Hol; Ethan A. Merritt

doi:10.1107/S1744309106005902

Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major

Tracy Arakaki
, Isolde Le Trong
, Eric Phizicky
, Erin Quartley
, George DeTitta
, Joseph Luft
, Angela Lauricella
, Lori Anderson
, Oleksandr Kalyuzhniy
, Elizabeth Worthey
, Peter J. Myler
, David Kim
, David Baker
, Wim G.J. Hol
, Ethan A. Merritt

Department of Structural Biology

University at Buffalo

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

The gene product of structural genomics target Lmaj006129 from Leishmania major codes for a 164-residue protein of unknown function. When SeMet expression of the full-length gene product failed, several truncation variants were created with the aid of Ginzu, a domain-prediction method. 11 truncations were selected for expression, purification and crystallization based upon secondary-structure elements and disorder. The structure of one of these variants, Lmaj006129AAH, was solved by multiple-wavelength anomalous diffraction (MAD) using ELVES, an automatic protein crystal structure-determination system. This model was then successfully used as a molecular-replacement probe for the parent full-length target, Lmaj006129AAA. The final structure of Lmaj006129AAA was refined to an R value of 0.185 (R_free = 0.229) at 1.60 Å resolution. Structure and sequence comparisons based on Lmaj006129AAA suggest that proteins belonging to Pfam sequence families PF04543 and PF01878 may share a common ligand-binding motif.

Original language	English
Pages (from-to)	175-179
Number of pages	5
Journal	Acta Crystallographica Section F: Structural Biology and Crystallization Communications
Volume	62
Issue number	3
DOIs	https://doi.org/10.1107/S1744309106005902
State	Published - 2006

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10.1107/S1744309106005902

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Arakaki, T., Le Trong, I., Phizicky, E., Quartley, E., DeTitta, G., Luft, J., Lauricella, A., Anderson, L., Kalyuzhniy, O., Worthey, E., Myler, P. J., Kim, D., Baker, D., Hol, W. G. J., & Merritt, E. A. (2006). Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major. Acta Crystallographica Section F: Structural Biology and Crystallization Communications, 62(3), 175-179. https://doi.org/10.1107/S1744309106005902

@article{beb5de3f96f04b9e9fc9ff743a826736,

title = "Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major",

abstract = "The gene product of structural genomics target Lmaj006129 from Leishmania major codes for a 164-residue protein of unknown function. When SeMet expression of the full-length gene product failed, several truncation variants were created with the aid of Ginzu, a domain-prediction method. 11 truncations were selected for expression, purification and crystallization based upon secondary-structure elements and disorder. The structure of one of these variants, Lmaj006129AAH, was solved by multiple-wavelength anomalous diffraction (MAD) using ELVES, an automatic protein crystal structure-determination system. This model was then successfully used as a molecular-replacement probe for the parent full-length target, Lmaj006129AAA. The final structure of Lmaj006129AAA was refined to an R value of 0.185 (Rfree = 0.229) at 1.60 {\AA} resolution. Structure and sequence comparisons based on Lmaj006129AAA suggest that proteins belonging to Pfam sequence families PF04543 and PF01878 may share a common ligand-binding motif.",

author = "Tracy Arakaki and \{Le Trong\}, Isolde and Eric Phizicky and Erin Quartley and George DeTitta and Joseph Luft and Angela Lauricella and Lori Anderson and Oleksandr Kalyuzhniy and Elizabeth Worthey and Myler, \{Peter J.\} and David Kim and David Baker and Hol, \{Wim G.J.\} and Merritt, \{Ethan A.\}",

year = "2006",

doi = "10.1107/S1744309106005902",

language = "English",

volume = "62",

pages = "175--179",

journal = "Acta Crystallographica Section F: Structural Biology and Crystallization Communications",

issn = "1744-3091",

publisher = "John Wiley and Sons Ltd",

number = "3",

}

Arakaki, T, Le Trong, I, Phizicky, E, Quartley, E, DeTitta, G, Luft, J, Lauricella, A, Anderson, L, Kalyuzhniy, O, Worthey, E, Myler, PJ, Kim, D, Baker, D, Hol, WGJ & Merritt, EA 2006, 'Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major', Acta Crystallographica Section F: Structural Biology and Crystallization Communications, vol. 62, no. 3, pp. 175-179. https://doi.org/10.1107/S1744309106005902

TY - JOUR

T1 - Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major

AU - Arakaki, Tracy

AU - Le Trong, Isolde

AU - Phizicky, Eric

AU - Quartley, Erin

AU - DeTitta, George

AU - Luft, Joseph

AU - Lauricella, Angela

AU - Anderson, Lori

AU - Kalyuzhniy, Oleksandr

AU - Worthey, Elizabeth

AU - Myler, Peter J.

AU - Kim, David

AU - Baker, David

AU - Hol, Wim G.J.

AU - Merritt, Ethan A.

PY - 2006

Y1 - 2006

N2 - The gene product of structural genomics target Lmaj006129 from Leishmania major codes for a 164-residue protein of unknown function. When SeMet expression of the full-length gene product failed, several truncation variants were created with the aid of Ginzu, a domain-prediction method. 11 truncations were selected for expression, purification and crystallization based upon secondary-structure elements and disorder. The structure of one of these variants, Lmaj006129AAH, was solved by multiple-wavelength anomalous diffraction (MAD) using ELVES, an automatic protein crystal structure-determination system. This model was then successfully used as a molecular-replacement probe for the parent full-length target, Lmaj006129AAA. The final structure of Lmaj006129AAA was refined to an R value of 0.185 (Rfree = 0.229) at 1.60 Å resolution. Structure and sequence comparisons based on Lmaj006129AAA suggest that proteins belonging to Pfam sequence families PF04543 and PF01878 may share a common ligand-binding motif.

AB - The gene product of structural genomics target Lmaj006129 from Leishmania major codes for a 164-residue protein of unknown function. When SeMet expression of the full-length gene product failed, several truncation variants were created with the aid of Ginzu, a domain-prediction method. 11 truncations were selected for expression, purification and crystallization based upon secondary-structure elements and disorder. The structure of one of these variants, Lmaj006129AAH, was solved by multiple-wavelength anomalous diffraction (MAD) using ELVES, an automatic protein crystal structure-determination system. This model was then successfully used as a molecular-replacement probe for the parent full-length target, Lmaj006129AAA. The final structure of Lmaj006129AAA was refined to an R value of 0.185 (Rfree = 0.229) at 1.60 Å resolution. Structure and sequence comparisons based on Lmaj006129AAA suggest that proteins belonging to Pfam sequence families PF04543 and PF01878 may share a common ligand-binding motif.

UR - https://www.scopus.com/pages/publications/33645729582

U2 - 10.1107/S1744309106005902

DO - 10.1107/S1744309106005902

M3 - Article

C2 - 16511295

SN - 1744-3091

VL - 62

SP - 175

EP - 179

JO - Acta Crystallographica Section F: Structural Biology and Crystallization Communications

JF - Acta Crystallographica Section F: Structural Biology and Crystallization Communications

IS - 3

ER -

Structure of Lmaj006129AAA, a hypothetical protein from Leishmania major

Abstract

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