INTERSTITIAL DELETIONS IN DIGEORGE SYNDROME DETECTED WITH MICROCLONES FROM 22Q11

被引：17

作者：

CAREY, AH

CLAUSSEN, U

LUDECKE, HJ

HORSTHEMKE, B

ELLIS, D

OAKEY, H

WILSON, D

BURN, J

WILLIAMSON, R

SCAMBLER, PJ

机构：

[1] UNIV LONDON IMPERIAL COLL SCI & TECHNOL, ST MARYS HOSP, SCH MED, DEPT BIOCHEM & MOLEC GENET, PADDINGTON W2 1PG, ENGLAND

[2] UNIV NEWCASTLE UPON TYNE, DIV HUMAN GENET, NEWCASTLE NE2 4AA, ENGLAND

[3] UNIV ERLANGEN NURNBERG, INST HUMANGENET, W-8520 ERLANGEN, GERMANY

[4] UNIV ESSEN GESAMTHSCH KLINIKUM, INST HUMANGENET, W-4300 ESSEN 1, GERMANY

来源：

MAMMALIAN GENOME | 1992年 / 3卷 / 02期

关键词：

D O I：

10.1007/BF00431253

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

DiGeorge syndrome in humans is characterized by immunodeficiency, heart defects, mental retardation and facial dysmorphism; cytogenetic analysis has shown that deletions at 22q11 occur in approximately 25% of cases. To generate DNA markers from this region, we have microdissected and microcloned band q11 of human Chromosome (Chr) 22. Nineteen thousand clones were obtained from material dissected from 20 chromosome fragments. Seventeen of 61 clones analyzed (28%) were repetitive, 27 (44%) gave no signal, and 17 (28%) detected single copy sequences of which ten mapped to Chr 22. Two of these were found to be deleted in patients with DiGeorge syndrome and either monosomy for 22q11-pter or visible interstitial deletions of 22q11. These two markers are also hemizygous in patients with no visible chromosomal abnormality, demonstrating that submicroscopic deletions are common in DiGeorge syndrome patients.

引用

页码：101 / 105

页数：5

共 19 条

[11] DETECTION OF MOLECULAR-REARRANGEMENTS IN PRADER-WILLI SYNDROME PATIENTS BY USING GENOMIC PROBES RECOGNIZING 4 LOCI WITHIN THE PWCR
GREGORY, CA
KIRKILIONIS, AJ
GREENBERG, CR
CHUDLEY, AE
HAMERTON, JL
[J]. AMERICAN JOURNAL OF MEDICAL GENETICS, 1990, 35 (04): : 536 - 545
[12] CONFIRMATION OF AUTOSOMAL DOMINANT TRANSMISSION OF THE DIGEORGE MALFORMATION COMPLEX
KEPPEN, LD
FASULES, JW
BURKS, AW
GOLLIN, SM
SAWYER, JR
MILLER, CH
[J]. JOURNAL OF PEDIATRICS, 1988, 113 (03) : 506 - 508
[13] NEURAL CREST CELLS CONTRIBUTE TO NORMAL AORTICOPULMONARY SEPTATION
KIRBY, ML
GALE, TF
STEWART, DE
[J]. SCIENCE, 1983, 220 (4601) : 1059 - 1061
[14] LUDECKE HJ, 1990, HUM GENET, V84, P512
[15] CLONING DEFINED REGIONS OF THE HUMAN GENOME BY MICRODISSECTION OF BANDED CHROMOSOMES AND ENZYMATIC AMPLIFICATION
LUDECKE, HJ
SENGER, G
CLAUSSEN, U
HORSTHEMKE, B
[J]. NATURE, 1989, 338 (6213) : 348 - 350
[16] MULLER W, 1988, EUR J PEDIATR, V147, P496
[17] FAMILIAL 3RD-4RT PHARYNGEAL POUCH SYNDROME WITH APPARENT AUTOSOMAL DOMINANT TRANSMISSION
ROHN, RD
LEFFELL, MS
LEADEM, P
JOHNSON, D
RUBIO, T
EMANUEL, BS
[J]. JOURNAL OF PEDIATRICS, 1984, 105 (01) : 47 - 51
[18] MICRODELETIONS WITHIN 22Q11 ASSOCIATED WITH SPORADIC AND FAMILIAL DIGEORGE SYNDROME
SCAMBLER, PJ
CAREY, AH
WYSE, RKH
ROACH, S
DUMANSKI, JP
NORDENSKJOLD, M
WILLIAMSON, R
[J]. GENOMICS, 1991, 10 (01) : 201 - 206
[19] SENGER G, 1990, HUM GENET, V84, P507

← 1 2 →