FAMILIAL AMYLOIDOSIS - A STUDY OF 52 NORTH AMERICAN-BORN PATIENTS EXAMINED DURING A 30-YEAR PERIOD

被引：72

作者：

GERTZ, MA ^{[1
]}

KYLE, RA ^{[1
]}

THIBODEAU, SN ^{[1
]}

机构：

[1] MAYO CLIN & MAYO FDN,LAB GENET SECT,ROCHESTER,MN 55905

来源：

MAYO CLINIC PROCEEDINGS | 1992年 / 67卷 / 05期

关键词：

D O I：

10.1016/S0025-6196(12)60388-7

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Between 1961 and 1990, 52 patients with biopsy-proven familial amyloidosis born in North America were examined at the Mayo Clinic. At the time of diagnosis of familial amyloidosis, 83% of these patients had peripheral neuropathy, 33% had autonomic neuropathy, and 27% had cardiomyopathy. Renal disease was noted in fewer than 10%, and liver involvement was rare. The median age at diagnosis was 64 years. The sensitivity of various diagnostic biopsies was similar to that for primary amyloidosis: deposits of amyloid were found in 77 and 78% of the subcutaneous fat aspirates or rectal biopsy specimens, respectively, and in 41 % of specimens of bone marrow. The median duration of survival of 5.8 years for patients with inherited amyloidosis was superior to that for patients with primary amyloidosis. When patients were stratified by organ involvement, the survival of patients with familial amyloidosis remained superior. The presence of cardiomyopathy and an interactive variable of age and the presence of autonomic neuropathy were powerful predictors of survival. Of the 52 patients, 22 died, 12 (55 %) of cardiac failure or cardiac arrhythmia. Nine patients (41 %) died of inanition in conjunction with progressive peripheral or autonomic neuropathy. Transthyretin was identified by immunohistochemical studies in 31 of the 34 tissue specimens tested. A transthyretin mutation was identified in 24 of the 31. A transthyretin mutation was found in five additional patients for whom tissue was unavailable for immunostaining.

引用

页码：428 / 440

页数：13

共 70 条

[1] CURRENT AND PROPOSED TREATMENT OF FAMILIAL AMYLOIDOTIC POLYNEUROPATHY [J].

ADACHI, N .

CLINICAL NEUROPHARMACOLOGY, 1989, 12 (06) :506-513

[2] BLEEDING MANIFESTATIONS IN 24 PATIENTS WITH FAMILIAL AMYLOIDOTIC POLYNEUROPATHY [J].

ADACHI, N ;

SHOJI, S ;

YANAGISAWA, N .

EUROPEAN NEUROLOGY, 1988, 28 (02) :115-116

[3]

ALMEIDA MR, 1990, HUM GENET, V85, P623

[4] ROLE OF VARIANT PREALBUMIN IN THE PATHOGENESIS OF FAMILIAL AMYLOIDOTIC POLYNEUROPATHY - FATE OF NORMAL AND VARIANT PREALBUMIN IN THE CIRCULATION [J].

ANDO, Y ;

IKEGAWA, S ;

MIYAZAKI, A ;

INOUE, M ;

MORINO, Y ;

ARAKI, S .

ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1989, 274 (01) :87-93

[5] A PECULIAR FORM OF PERIPHERAL NEUROPATHY - FAMILIAR ATYPICAL GENERALIZED AMYLOIDOSIS WITH SPECIAL INVOLVEMENT OF THE PERIPHERAL NERVES [J].

ANDRADE, C .

BRAIN, 1952, 75 (03) :408-427

[6] TREATMENT BY PACEMAKER IN FAMILIAL AMYLOID POLYNEUROPATHY [J].

ANZAI, N ;

AKIYAMA, K ;

TSUCHIDA, K ;

YAMADA, M ;

KITO, S ;

YAMAMURA, Y .

CHEST, 1989, 96 (01) :80-84

[7] STUDIES OF NEUROCIRCULATORY EFFECTS OF LONG-TERM L-THREO-3,4-DIHYDROXYPHENYLSERINE ADMINISTRATION IN A PATIENT WITH FAMILIAL AMYLOIDOTIC POLYNEUROPATHY [J].

AZUMA, T ;

SUZUKI, T ;

MIZUNO, R ;

TSUJINO, S ;

KISHIMOTO, S ;

MIZUTA, E ;

ICHIKAWA, K .

ACTA NEUROLOGICA SCANDINAVICA, 1988, 77 (05) :409-413

[8] ELECTROPHYSIOLOGIC EVALUATION OF THE CARDIAC CONDUCTION SYSTEM AND ITS AUTONOMIC REGULATION IN FAMILIAL AMYLOID POLYNEUROPATHY [J].

BERGFELDT, BL ;

OLOFSSON, BO ;

EDHAG, KO .

AMERICAN JOURNAL OF CARDIOLOGY, 1985, 56 (10) :647-652

[9] THE TRANSTHYRETIN CDNA SEQUENCE IS NORMAL IN TRANSTHYRETIN-DERIVED SENILE SYSTEMIC AMYLOIDOSIS [J].

CHRISTMANSON, L ;

BETSHOLTZ, C ;

GUSTAVSSON, A ;

JOHANSSON, B ;

SLETTEN, K ;

WESTERMARK, P .

FEBS LETTERS, 1991, 281 (1-2) :177-180

[10] EVIDENCE THAT THE AMYLOID FIBRIL PROTEIN IN SENILE SYSTEMIC AMYLOIDOSIS IS DERIVED FROM NORMAL PREALBUMIN [J].

CORNWELL, GG ;

SLETTEN, K ;

JOHANSSON, B ;

WESTERMARK, P .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1988, 154 (02) :648-653

← 1 2 3 4 5 6 7 →