Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients.

Viacheslav N Kalinin; Jussuf Kaifi; Heidi Schwarzenbach; Anatoly S Sergeyev; Bjoern C Link; Dean Bogoevski; Yogesh Vashist; Jakob R Izbicki; Emre F Yekebas

Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients.

Standard

Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients. / Kalinin, Viacheslav N; Kaifi, Jussuf; Schwarzenbach, Heidi; Sergeyev, Anatoly S; Link, Bjoern C; Bogoevski, Dean; Vashist, Yogesh; Izbicki, Jakob R; Yekebas, Emre F.

in: WORLD J GASTROENTERO, Jahrgang 12, Nr. 33, 33, 2006, S. 5352-5356.

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

Harvard

Kalinin, VN, Kaifi, J, Schwarzenbach, H, Sergeyev, AS, Link, BC, Bogoevski, D, Vashist, Y, Izbicki, JR & Yekebas, EF 2006, 'Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients.', WORLD J GASTROENTERO, Jg. 12, Nr. 33, 33, S. 5352-5356. <http://www.ncbi.nlm.nih.gov/pubmed/16981266?dopt=Citation>

APA

Kalinin, V. N., Kaifi, J., Schwarzenbach, H., Sergeyev, A. S., Link, B. C., Bogoevski, D., Vashist, Y., Izbicki, J. R., & Yekebas, E. F. (2006). Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients. WORLD J GASTROENTERO, 12(33), 5352-5356. [33]. http://www.ncbi.nlm.nih.gov/pubmed/16981266?dopt=Citation

Vancouver

Kalinin VN, Kaifi J, Schwarzenbach H, Sergeyev AS, Link BC, Bogoevski D et al. Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients. WORLD J GASTROENTERO. 2006;12(33):5352-5356. 33.

Bibtex

@article{71c74ff2ba4e43c79235f17230f745c2,

title = "Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients.",

abstract = "AIM: To verify and expand the known spectrum of serine protease inhibitor Kazal type 1 (SPINK1) gene mutations in chronic pancreatitis. METHODS: DNA extracted from 172 chronic pancreatitis patients was assayed for SPINK1 gene mutations by PCR and DNA sequencing. A control cohort of 90 unrelated healthy individuals was analysed by the same methods for presence of common populational polymorphisms, and frequency of five-loci haplotypes was calculated. Linkages of gene aberrations in single SPINK1 gene copies were analysed by long-distance PCR followed by allele-specific PCR and DNA sequencing. RESULTS: The most frequent SPINK1 gene mutation N34S was found at a frequency of 6%. Furthermore, we detected the heterozygous intervening sequence (IVS) 3 + 2 T > C mutated gene in 2 German patients and 1 Macedonian chronic pancreatitis patient. In all three SPINK1 gene copies an additional rare base substitution was found: 5'untranslated region (UTR)-215 G > A. Polymorphism analysis revealed that all three affected genes carried the same five-loci haplotype. DNA sequencing of another chronic pancreatitis-related gene PRSS1 (cationic trypsinogen) did not reveal any mutations in these 3 patients. CONCLUSION: We found in 3 (2%) of 172 chronic pancreatitis patients an IVS3 + 2 T > C SPINK1 gene mutation and a base substitution 5'UTR-215 G > A in the same gene copy. Most probably the 5'UTR-215 G > A represents a rare polymorphism and not a mutation as previously concluded. Haplotype analysis suggests a common origin of the IVS3 + 2 T > C mutation in these patients.",

author = "Kalinin, {Viacheslav N} and Jussuf Kaifi and Heidi Schwarzenbach and Sergeyev, {Anatoly S} and Link, {Bjoern C} and Dean Bogoevski and Yogesh Vashist and Izbicki, {Jakob R} and Yekebas, {Emre F}",

year = "2006",

language = "Deutsch",

volume = "12",

pages = "5352--5356",

journal = "WORLD J GASTROENTERO",

issn = "1007-9327",

publisher = "WJG Press",

number = "33",

}

RIS

TY - JOUR

T1 - Association of rare SPINK1 gene mutation with another base substitution in chronic pancreatitis patients.

AU - Kalinin, Viacheslav N

AU - Kaifi, Jussuf

AU - Schwarzenbach, Heidi

AU - Sergeyev, Anatoly S

AU - Link, Bjoern C

AU - Bogoevski, Dean

AU - Vashist, Yogesh

AU - Izbicki, Jakob R

AU - Yekebas, Emre F

PY - 2006

Y1 - 2006

N2 - AIM: To verify and expand the known spectrum of serine protease inhibitor Kazal type 1 (SPINK1) gene mutations in chronic pancreatitis. METHODS: DNA extracted from 172 chronic pancreatitis patients was assayed for SPINK1 gene mutations by PCR and DNA sequencing. A control cohort of 90 unrelated healthy individuals was analysed by the same methods for presence of common populational polymorphisms, and frequency of five-loci haplotypes was calculated. Linkages of gene aberrations in single SPINK1 gene copies were analysed by long-distance PCR followed by allele-specific PCR and DNA sequencing. RESULTS: The most frequent SPINK1 gene mutation N34S was found at a frequency of 6%. Furthermore, we detected the heterozygous intervening sequence (IVS) 3 + 2 T > C mutated gene in 2 German patients and 1 Macedonian chronic pancreatitis patient. In all three SPINK1 gene copies an additional rare base substitution was found: 5'untranslated region (UTR)-215 G > A. Polymorphism analysis revealed that all three affected genes carried the same five-loci haplotype. DNA sequencing of another chronic pancreatitis-related gene PRSS1 (cationic trypsinogen) did not reveal any mutations in these 3 patients. CONCLUSION: We found in 3 (2%) of 172 chronic pancreatitis patients an IVS3 + 2 T > C SPINK1 gene mutation and a base substitution 5'UTR-215 G > A in the same gene copy. Most probably the 5'UTR-215 G > A represents a rare polymorphism and not a mutation as previously concluded. Haplotype analysis suggests a common origin of the IVS3 + 2 T > C mutation in these patients.

AB - AIM: To verify and expand the known spectrum of serine protease inhibitor Kazal type 1 (SPINK1) gene mutations in chronic pancreatitis. METHODS: DNA extracted from 172 chronic pancreatitis patients was assayed for SPINK1 gene mutations by PCR and DNA sequencing. A control cohort of 90 unrelated healthy individuals was analysed by the same methods for presence of common populational polymorphisms, and frequency of five-loci haplotypes was calculated. Linkages of gene aberrations in single SPINK1 gene copies were analysed by long-distance PCR followed by allele-specific PCR and DNA sequencing. RESULTS: The most frequent SPINK1 gene mutation N34S was found at a frequency of 6%. Furthermore, we detected the heterozygous intervening sequence (IVS) 3 + 2 T > C mutated gene in 2 German patients and 1 Macedonian chronic pancreatitis patient. In all three SPINK1 gene copies an additional rare base substitution was found: 5'untranslated region (UTR)-215 G > A. Polymorphism analysis revealed that all three affected genes carried the same five-loci haplotype. DNA sequencing of another chronic pancreatitis-related gene PRSS1 (cationic trypsinogen) did not reveal any mutations in these 3 patients. CONCLUSION: We found in 3 (2%) of 172 chronic pancreatitis patients an IVS3 + 2 T > C SPINK1 gene mutation and a base substitution 5'UTR-215 G > A in the same gene copy. Most probably the 5'UTR-215 G > A represents a rare polymorphism and not a mutation as previously concluded. Haplotype analysis suggests a common origin of the IVS3 + 2 T > C mutation in these patients.

M3 - SCORING: Zeitschriftenaufsatz

VL - 12

SP - 5352

EP - 5356

JO - WORLD J GASTROENTERO

JF - WORLD J GASTROENTERO

SN - 1007-9327

IS - 33

M1 - 33

ER -