Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types

Oyunbaatar Altanbayar; Avarzed Amgalanbaatar; Chimeddorj Battogtokh; Narmandakh Bayarjargal; Dana Belick; Malte Kohns Vasconcelos; Colin R Mackenzie; Klaus Pfeffer; Birgit Henrich

doi:10.1016/j.ijmm.2022.151552

Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types

Standard

Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types. / Altanbayar, Oyunbaatar; Amgalanbaatar, Avarzed; Battogtokh, Chimeddorj; Bayarjargal, Narmandakh; Belick, Dana; Kohns Vasconcelos, Malte; Mackenzie, Colin R; Pfeffer, Klaus; Henrich, Birgit.

in: INT J MED MICROBIOL, Jahrgang 312, Nr. 3, 04.2022, S. 151552.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Altanbayar, O, Amgalanbaatar, A, Battogtokh, C, Bayarjargal, N, Belick, D, Kohns Vasconcelos, M, Mackenzie, CR, Pfeffer, K & Henrich, B 2022, 'Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types', INT J MED MICROBIOL, Jg. 312, Nr. 3, S. 151552. https://doi.org/10.1016/j.ijmm.2022.151552

APA

Altanbayar, O., Amgalanbaatar, A., Battogtokh, C., Bayarjargal, N., Belick, D., Kohns Vasconcelos, M., Mackenzie, C. R., Pfeffer, K., & Henrich, B. (2022). Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types. INT J MED MICROBIOL, 312(3), 151552. https://doi.org/10.1016/j.ijmm.2022.151552

Vancouver

Altanbayar O, Amgalanbaatar A, Battogtokh C, Bayarjargal N, Belick D, Kohns Vasconcelos M et al. Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types. INT J MED MICROBIOL. 2022 Apr;312(3):151552. https://doi.org/10.1016/j.ijmm.2022.151552

Bibtex

@article{4f967f1d51cd470f84f135b5bbda95fb,

title = "Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types",

abstract = "Helicobacter pylori infection is strongly associated with gastritis, gastroduodenal ulcer disease and gastric carcinoma. The virulence of H. pylori strains increases with the presence of the pathogenicity island PAI, which encodes a Type 4 Secretion System and the oncoprotein CagA. Two major CagA types can be distinguished by differences in the repetitive EPIYA region in the C-terminal sequence; the more virulent East Asian CagA type with EPIYA-A, -B, and -D motifs and the Western CagA type with EPIYA-A, -B, and C motifs, the virulence of which is associated with the multitude of EPIYA-C motifs. In this study, the cagA gene was characterized in H. pylori strains isolated from Mongolians suffering from gastritis (80%) or ulcer (20%). The EPIYA region of 53 isolates was determined by PCR-amplification of overlapping cagA regions and subsequent Sanger sequencing. Only one H. pylori isolate carried the East Asian type (ABD) and 52 isolates the Western type of CagA, thereof 30 the EPIYA type ABC, 19 the ABCC type and one each of type ABCCCC, AAABC and AAAAB. An amino acid exchange from EPIYA-B to EPIYT-B was predominantly found in CagA proteins in strains with < 2 EPIYA-C copies (n = 25/32; p = 0.015) including the two EPIYA-A enriched CagA proteins, which have not been described to date. Due to the amino acid triplet preceding the EPIYA motif and strength of predicted phosphorylation, the multiple EPIYA-A motifs A2, A3 and A4 were shown to cluster with EPIYA-B and EPIYT-B with the unique feature of amino acid E in position - 4 to Y of EPIYA. It has been described that tyrosine-phosphorylated EPIYA-A and -B motifs counteract the EPIYA-C-driven signaling towards host cell transformation and malignancy. Thus, Mongolian H. pylori strains carrying CagA proteins not only with a few EPIYA-C segments but also with multiplied EPIYA-A segments are probably less virulent; a thesis that needs further investigation at the protein level.",

keywords = "Amino Acid Motifs, Antigens, Bacterial/genetics, Bacterial Proteins/metabolism, Helicobacter Infections, Helicobacter pylori, Humans, Mongolia",

author = "Oyunbaatar Altanbayar and Avarzed Amgalanbaatar and Chimeddorj Battogtokh and Narmandakh Bayarjargal and Dana Belick and {Kohns Vasconcelos}, Malte and Mackenzie, {Colin R} and Klaus Pfeffer and Birgit Henrich",

year = "2022",

month = apr,

doi = "10.1016/j.ijmm.2022.151552",

language = "English",

volume = "312",

pages = "151552",

journal = "INT J MED MICROBIOL",

issn = "1438-4221",

publisher = "Urban und Fischer Verlag GmbH und Co. KG",

number = "3",

}

RIS

TY - JOUR

T1 - Characterization of the cagA-gene in Helicobacter pylori in Mongolia and detection of two EPIYA-A enriched CagA types

AU - Altanbayar, Oyunbaatar

AU - Amgalanbaatar, Avarzed

AU - Battogtokh, Chimeddorj

AU - Bayarjargal, Narmandakh

AU - Belick, Dana

AU - Kohns Vasconcelos, Malte

AU - Mackenzie, Colin R

AU - Pfeffer, Klaus

AU - Henrich, Birgit

PY - 2022/4

Y1 - 2022/4

N2 - Helicobacter pylori infection is strongly associated with gastritis, gastroduodenal ulcer disease and gastric carcinoma. The virulence of H. pylori strains increases with the presence of the pathogenicity island PAI, which encodes a Type 4 Secretion System and the oncoprotein CagA. Two major CagA types can be distinguished by differences in the repetitive EPIYA region in the C-terminal sequence; the more virulent East Asian CagA type with EPIYA-A, -B, and -D motifs and the Western CagA type with EPIYA-A, -B, and C motifs, the virulence of which is associated with the multitude of EPIYA-C motifs. In this study, the cagA gene was characterized in H. pylori strains isolated from Mongolians suffering from gastritis (80%) or ulcer (20%). The EPIYA region of 53 isolates was determined by PCR-amplification of overlapping cagA regions and subsequent Sanger sequencing. Only one H. pylori isolate carried the East Asian type (ABD) and 52 isolates the Western type of CagA, thereof 30 the EPIYA type ABC, 19 the ABCC type and one each of type ABCCCC, AAABC and AAAAB. An amino acid exchange from EPIYA-B to EPIYT-B was predominantly found in CagA proteins in strains with < 2 EPIYA-C copies (n = 25/32; p = 0.015) including the two EPIYA-A enriched CagA proteins, which have not been described to date. Due to the amino acid triplet preceding the EPIYA motif and strength of predicted phosphorylation, the multiple EPIYA-A motifs A2, A3 and A4 were shown to cluster with EPIYA-B and EPIYT-B with the unique feature of amino acid E in position - 4 to Y of EPIYA. It has been described that tyrosine-phosphorylated EPIYA-A and -B motifs counteract the EPIYA-C-driven signaling towards host cell transformation and malignancy. Thus, Mongolian H. pylori strains carrying CagA proteins not only with a few EPIYA-C segments but also with multiplied EPIYA-A segments are probably less virulent; a thesis that needs further investigation at the protein level.

AB - Helicobacter pylori infection is strongly associated with gastritis, gastroduodenal ulcer disease and gastric carcinoma. The virulence of H. pylori strains increases with the presence of the pathogenicity island PAI, which encodes a Type 4 Secretion System and the oncoprotein CagA. Two major CagA types can be distinguished by differences in the repetitive EPIYA region in the C-terminal sequence; the more virulent East Asian CagA type with EPIYA-A, -B, and -D motifs and the Western CagA type with EPIYA-A, -B, and C motifs, the virulence of which is associated with the multitude of EPIYA-C motifs. In this study, the cagA gene was characterized in H. pylori strains isolated from Mongolians suffering from gastritis (80%) or ulcer (20%). The EPIYA region of 53 isolates was determined by PCR-amplification of overlapping cagA regions and subsequent Sanger sequencing. Only one H. pylori isolate carried the East Asian type (ABD) and 52 isolates the Western type of CagA, thereof 30 the EPIYA type ABC, 19 the ABCC type and one each of type ABCCCC, AAABC and AAAAB. An amino acid exchange from EPIYA-B to EPIYT-B was predominantly found in CagA proteins in strains with < 2 EPIYA-C copies (n = 25/32; p = 0.015) including the two EPIYA-A enriched CagA proteins, which have not been described to date. Due to the amino acid triplet preceding the EPIYA motif and strength of predicted phosphorylation, the multiple EPIYA-A motifs A2, A3 and A4 were shown to cluster with EPIYA-B and EPIYT-B with the unique feature of amino acid E in position - 4 to Y of EPIYA. It has been described that tyrosine-phosphorylated EPIYA-A and -B motifs counteract the EPIYA-C-driven signaling towards host cell transformation and malignancy. Thus, Mongolian H. pylori strains carrying CagA proteins not only with a few EPIYA-C segments but also with multiplied EPIYA-A segments are probably less virulent; a thesis that needs further investigation at the protein level.

KW - Amino Acid Motifs

KW - Antigens, Bacterial/genetics

KW - Bacterial Proteins/metabolism

KW - Helicobacter Infections

KW - Helicobacter pylori

KW - Humans

KW - Mongolia

U2 - 10.1016/j.ijmm.2022.151552

DO - 10.1016/j.ijmm.2022.151552

M3 - SCORING: Journal article

C2 - 35231822

VL - 312

SP - 151552

JO - INT J MED MICROBIOL

JF - INT J MED MICROBIOL

SN - 1438-4221

IS - 3

ER -