Amylo-l,6-glucosidase deficiency 19 it is obvious that a diagnosis of heterozygosity cannot be estab- ished in singie individuals by this method. Healthy sibs of patients (with a chance of being heterozygous of 67 °/o) and sibs of parents of patients (with a chance of heterozygosity around 50 °/o) have as expected medial values between those seen in definite heterozygotes and in normals. The determination of enzyme activity in the erythrocytes does not permit any distinction between patients and definite heterozygotes. It is possible that the presence of measurable activity in the patients is an artifact due to unspecific binding of radioactive glucose to glycogen and protein in the assay; this may also take place in the assay of the enzyme in leuco- cytes, but the results here show zero activity in the patients, corresponding to the much lower protein concentration ín this assay. The median value of erythrocyte activity in normals is much higher than that of the patients and the heterozygotes, but the distributions overlap considerably. Thus, the examina- tion of erythrocytes by the methods adopted here is less in- formative than the study of leucocyte activity. It seems clear that more reliable methods of defining hetero- zygotes are needed for practical as well as theoretical purposes. Genetic counselling cannot be sufficiently exact as long as such methods are lacking, and they will be needed if more effective preventive measures such as screening of newborns in this and other high risk populations are to be introduced. Linkage ana- lyses would also have to await the appearance of methods for reliable heterozygote detection. The present suggestion of a possible association between the gene determining ADA vari- ants and enzyme activity may be due to chance alone as a considerable number of tests for association was performed. It might, however, be worthwile to attempt studies of the genetic relation between the genetic ADA variation and amylo- 1,6-glucosidase deficiency by somatic cell hybridization; posi- tive results obtained in this way could be of high value in the continued studies which aim at a more complete elucidation of type III glycogenosis.

Side 1
Side 2
Side 3
Side 4
Side 5
Side 6
Side 7
Side 8
Side 9
Side 10
Side 11
Side 12
Side 13
Side 14
Side 15
Side 16
Side 17
Side 18
Side 19
Side 20
Side 21
Side 22
Side 23
Side 24
Side 25
Side 26
Side 27
Side 28
Side 29
Side 30
Side 31
Side 32
Side 33
Side 34
Side 35
Side 36
Side 37
Side 38
Side 39
Side 40
Side 41
Side 42
Side 43
Side 44
Side 45
Side 46
Side 47
Side 48
Side 49
Side 50
Side 51
Side 52
Side 53
Side 54
Side 55
Side 56
Side 57
Side 58
Side 59
Side 60
Side 61
Side 62
Side 63
Side 64
Side 65
Side 66
Side 67
Side 68
Side 69
Side 70
Side 71
Side 72
Side 73
Side 74
Side 75
Side 76
Side 77
Side 78
Side 79
Side 80
Side 81
Side 82
Side 83
Side 84
Side 85
Side 86
Side 87
Side 88
Side 89
Side 90
Side 91
Side 92
Side 93
Side 94
Side 95
Side 96
Side 97
Side 98
Side 99
Side 100
Side 101
Side 102
Side 103
Side 104
Side 105
Side 106
Side 107
Side 108
Side 109
Side 110
Side 111
Side 112