PEARSON MARROW PANCREAS SYNDROME - A MULTISYSTEM MITOCHONDRIAL DISORDER IN INFANCY

被引：385

作者：

ROTIG, A

CORMIER, V

BLANCHE, S

BONNEFONT, JP

LEDEIST, F

ROMERO, N

SCHMITZ, J

RUSTIN, P

FISCHER, A

SAUDUBRAY, JM

MUNNICH, A

机构：

[1] INSERM,U12,UNITE RECH HANDICAPS GENET ENFANT,F-75743 PARIS,FRANCE

[2] HOP ENFANTS MALAD,DEPT PEDIAT,F-75743 PARIS,FRANCE

[3] INSERM,U153,UNITE RECH BIOL & PATHOL NEUROMUSCULAIRES,F-75005 PARIS,FRANCE

来源：

JOURNAL OF CLINICAL INVESTIGATION | 1990年 / 86卷 / 05期

关键词：

lactate/pyruvate molar ratios; mitochondrial cytopathies; Pearson's syndrome; rearrangement of the mitochondrial DNA;

D O I：

10.1172/JCI114881

中图分类号：

R-3 [医学研究方法]; R3 [基础医学];

学科分类号：

1001 ;

摘要：

Pearson's marrow-pancreas syndrome (McKusick No. 26056) is a fatal disorder of hitherto unknown etiology involving the hematopoietic system, exocrine pancreas, liver, and kidneys. The observation of high lactate/pyruvate molar ratios in plasma and abnormal oxidative phosphorylation in lymphocytes led us to postulate that Pearson's syndrome belongs to the group of mitochondrial cytopathies. Since rearrangements of the mitochondrial genome between direct DNA repeats were consistently found in all tissues tested, our results show that this disease is in fact a multisystem mitochondrial disorder, as suggested by the clinical course of the patients. Based on these observations, we would suggest giving consideration to the hypothesis of a defect of oxidative phosphorylation in elucidating the origin of other syndromes, especially those associated with an abnormal oxidoreduction status in plasma.

引用

页码：1601 / 1608

页数：8

共 25 条

[1] ON THE FORMATION OF SPONTANEOUS DELETIONS - THE IMPORTANCE OF SHORT SEQUENCE HOMOLOGIES IN THE GENERATION OF LARGE DELETIONS
ALBERTINI, AM
HOFER, M
CALOS, MP
MILLER, JH
[J]. CELL, 1982, 29 (02) : 319 - 328
[2] SEQUENCE AND ORGANIZATION OF THE HUMAN MITOCHONDRIAL GENOME
ANDERSON, S
BANKIER, AT
BARRELL, BG
DEBRUIJN, MHL
COULSON, AR
DROUIN, J
EPERON, IC
NIERLICH, DP
ROE, BA
SANGER, F
SCHREIER, PH
SMITH, AJH
STADEN, R
YOUNG, IG
[J]. NATURE, 1981, 290 (5806) : 457 - 465
[3] MEASUREMENT OF CYTOCHROMES IN HUMAN SKELETAL-MUSCLE MITOCHONDRIA, ISOLATED FROM FRESH AND FROZEN STORED MUSCLE SPECIMENS
BOOKELMAN, H
TRIJBELS, JMF
SENGERS, RCA
JANSSEN, AJM
[J]. BIOCHEMICAL MEDICINE, 1978, 19 (03): : 366 - 373
[4] BOYUM A, 1968, J CLIN LAB INVES S97, V21, P245
[5] Dubowitz V., 1973, MUSCLE BIOPSY MODERN
[6] Dujon B., 1989, MOBILE DNA, P861
[7] SPECIFIC DNA AMPLIFICATION
ERLICH, HA
GELFAND, DH
SAIKI, RK
[J]. NATURE, 1988, 331 (6155) : 461 - 462
[8] Estabrook R., 1967, METHOD ENZYMOL, V10, P41, DOI DOI 10.1016/0076-6879(67)10010-4
[9] MATERNAL INHERITANCE OF HUMAN MITOCHONDRIAL-DNA
GILES, RE
BLANC, H
CANN, HM
WALLACE, DC
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1980, 77 (11): : 6715 - 6719
[10] DELETIONS OF MUSCLE MITOCHONDRIAL-DNA IN MITOCHONDRIAL MYOPATHIES - SEQUENCE-ANALYSIS AND POSSIBLE MECHANISMS
HOLT, IJ
HARDING, AE
MORGANHUGHES, JA
[J]. NUCLEIC ACIDS RESEARCH, 1989, 17 (12) : 4465 - 4469

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