Hereditary amyloidosis

Andrade, Carla Sousa; Araki, Shukuro; Block, Walter D.; Cohen, Alan S.; Jackson, Charles E.; Kuroiwa, Yoshigoro; McKusick, Victor A.; Nissim, J.; Sohar, Ezra; Allen, Maurice W. Van

doi:10.1002/art.1780130622

Cited by 76 publications

(34 citation statements)

References 37 publications

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“…The finding that the relatively rare variants of two genetic markers in Japan, Gc*IA2 and PGMI*7, are distributed over the three genealogically independent families suggests that the families (Sa, U and Tu) may have a common ancester. Phenotypes attributable to Caucasians, for example K+ in the Kell blood group, were not found in the present study and hence no evidence was found for the hypothesis that the FAP gene in Arao was derived from the Portuguese (Andrade et al, 1970). Whether a few rather unusual findings in the ABO blood groups, the Kidd groups, the Hp and the Pi systems, reflect only the characteristics of FAP in the Arao district or that of FAP itself remains to be solved.…”

Section: Discussioncontrasting

confidence: 77%

“…The disease has a curious geographic distribution: there are large foci in Portugal (Andrade et al, 1969), Sweden (Andersson, 1976), and Japan (Araki et al, 1968;Kito et al, 1973), but the disease is uncommon elsewhere. Whether FAP in Japan has a Portuguese ancestry or not is an interesting enigma (Andrade et al, 1970). In a previous paper (Sakoda et al, 1983), we reported genealogical studies of FAP in the Arao district of Kumamoto prefecture.…”

Section: Introductionmentioning

confidence: 96%

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The genetic studies of familial amyloid polyneuropathy in the Arao district of Japan: II. Studies of genetic markers in blood

et al. 1984

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SummaryBlood samples from 21 patients with familial amyloid polyneuropathy (FAP) and 81 normal family members among 7 affected families in Arao were tested for 9 blood group systems, 8 serum polymorphic proteins, 12 red cell polymorphic enzymes, and HLA. One of the most important findings was the existence of two relatively rare variants, i.e., group specific component Gc*IA2 and phosphoglucomutase PGMI*7 in 3 families. This observation suggests that the three genealogically independent families may have a common ancester. Phenotype AB in the ABO blood group system, phenotype 1 in the haptoglobin system, and M2 gene in the protease inhibitor system were not seen, and phenotype Jk(a+b-) in the Kidd groups was found in only one patient. Whether these observations reflect the characteristics of FAP in the Arao district or that of FAP itself can not be determined from the present study. No phenotype attributable to Caucasians was found, hence the study provides no support for the hypothesis that the gene for FAP was introduced into Japan by the Portuguese.

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Section: Discussioncontrasting

confidence: 77%

Section: Introductionmentioning

confidence: 96%

The genetic studies of familial amyloid polyneuropathy in the Arao district of Japan: II. Studies of genetic markers in blood

et al. 1984

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“…phosphogluc0mutase 7 and group specific component J (Sakoda et al, 1984), we can conclude that five of the nine families have a common ancestor. Whether or not 'the FAP gene in the Arao focuS is derived from the Protuguese reamins an interesting enigma (Andrade et al, 1970): Second, it lends credence to the view that the prealbumin variant is essentially concerned with the pathogenic mechanism of this gerteticatly determined neuropathic disease. Although Tawara et aL: (1983) .~oL 29,, No;',:,3,, 1984 reserved an alternative possibility-that this prealbumin variant is a polymorphism of prealbumin, the findings of this study make it unlikely.…”

Section: Discussionmentioning

confidence: 96%

Genetic studies of familial amyloid polyneuropathy in the Arao district of Japan

et al. 1984

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“…Extensive genetic studies have failed to reveal connection with any of the several kindreds with amyloidosis in the United States or with Portuguese kindreds (8).…”

Section: Discussionmentioning

confidence: 99%

“…Classical secondary amyloidosis associated with chronic inflammatory diseases has deposits that are composed of amyloid A (AA),' a degradation product of an acute phase reactant, serum AA (SAA) (6,7). A third commonly recognized type of systemic amyloidosis is seen with the heredofamilial syndromes (8).…”

Section: Introductionmentioning

confidence: 99%

Partial amino acid sequence homology between an heredofamilial amyloid protein and human plasma prealbumin.

Benson¹

1981

J. Clin. Invest.

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Hereditary amyloidosis

Cited by 76 publications

References 37 publications

The genetic studies of familial amyloid polyneuropathy in the Arao district of Japan: II. Studies of genetic markers in blood

The genetic studies of familial amyloid polyneuropathy in the Arao district of Japan: II. Studies of genetic markers in blood

Genetic studies of familial amyloid polyneuropathy in the Arao district of Japan

Partial amino acid sequence homology between an heredofamilial amyloid protein and human plasma prealbumin.

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