10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE).

Rudolf Erttmann; T Tafese; F Berthold; R Kerbl; J Mann; L Parker; F Schilling; P Ambros; H Christiansen; M Favrot; H Kabisch; B Hero; T Philip

10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE).

Standard

10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE). / Erttmann, Rudolf; Tafese, T; Berthold, F; Kerbl, R; Mann, J; Parker, L; Schilling, F; Ambros, P; Christiansen, H; Favrot, M; Kabisch, H; Hero, B; Philip, T.

In: EUR J CANCER, Vol. 34, No. 9, 9, 1998, p. 1391-1397.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Erttmann, R, Tafese, T, Berthold, F, Kerbl, R, Mann, J, Parker, L, Schilling, F, Ambros, P, Christiansen, H, Favrot, M, Kabisch, H, Hero, B & Philip, T 1998, '10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE).', EUR J CANCER, vol. 34, no. 9, 9, pp. 1391-1397. <http://www.ncbi.nlm.nih.gov/pubmed/9849422?dopt=Citation>

APA

Erttmann, R., Tafese, T., Berthold, F., Kerbl, R., Mann, J., Parker, L., Schilling, F., Ambros, P., Christiansen, H., Favrot, M., Kabisch, H., Hero, B., & Philip, T. (1998). 10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE). EUR J CANCER, 34(9), 1391-1397. [9]. http://www.ncbi.nlm.nih.gov/pubmed/9849422?dopt=Citation

Vancouver

Erttmann R, Tafese T, Berthold F, Kerbl R, Mann J, Parker L et al. 10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE). EUR J CANCER. 1998;34(9):1391-1397. 9.

Bibtex

@article{e3274e217f8946c397ca7b9a31bd7971,

title = "10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE).",

abstract = "Between January 1986 and May 1996, 870,313 children were tested in European neuroblastoma (NB) screening programmes. Among these children, 82 cases of NB (age range 4-24 months, median 11 months) were detected by screening. 83% of the patients had localised NB and 17% were diagnosed with generalised NB (stage 4, 10%; stage 4s, 7%). Unfavourable biological markers (MYCN amplification, loss of heterozygosity (LOH) 1p36, DNA di/tetraploidy) were observed in 14% of 76 biologically examined cases. The median follow-up time of all the patients was 21.5 months (range 1-101 months). To date, 69 patients are in complete remission (CR) and 2 patients have died due to therapy (stage 4, 1 patient; stage 3, 1 patient with unfavourable markers). Apart from screened patients, 16 other patients with NB were found who had previously had a normal screening test, i.e. 'false negative' patients (age range 10-41 months, median 31.5 months). The median interval between screening and diagnosis was 24.5 months (range 6-35 months). 11 of the 'false negative' patients suffered from generalised NB (stage 4) and 5 had localised NB at diagnosis. Unfavourable biological markers were observed in 7/12 patients. 5 patients have died, 2 achieved partial remission and 9 CR. 9 of the 11 patients with unfavourable biological markers diagnosed due to NB screening are currently in CR. It is very likely that, among the patients without unfavourable biological markers, we detected tumours which may have regressed spontaneously. These children may have undergone 'unnecessary,' but unavoidable, diagnostic procedures and therapy. To reduce the number of 'false negative' patients, a later screening could be helpful and should be evaluated.",

author = "Rudolf Erttmann and T Tafese and F Berthold and R Kerbl and J Mann and L Parker and F Schilling and P Ambros and H Christiansen and M Favrot and H Kabisch and B Hero and T Philip",

year = "1998",

language = "Deutsch",

volume = "34",

pages = "1391--1397",

journal = "EUR J CANCER",

issn = "0959-8049",

publisher = "Elsevier Limited",

number = "9",

}

RIS

TY - JOUR

T1 - 10 years' neuroblastoma screening in Europe: preliminary results of a clinical and biological review from the Study Group for Evaluation of Neuroblastoma Screening in Europe (SENSE).

AU - Erttmann, Rudolf

AU - Tafese, T

AU - Berthold, F

AU - Kerbl, R

AU - Mann, J

AU - Parker, L

AU - Schilling, F

AU - Ambros, P

AU - Christiansen, H

AU - Favrot, M

AU - Kabisch, H

AU - Hero, B

AU - Philip, T

PY - 1998

Y1 - 1998

N2 - Between January 1986 and May 1996, 870,313 children were tested in European neuroblastoma (NB) screening programmes. Among these children, 82 cases of NB (age range 4-24 months, median 11 months) were detected by screening. 83% of the patients had localised NB and 17% were diagnosed with generalised NB (stage 4, 10%; stage 4s, 7%). Unfavourable biological markers (MYCN amplification, loss of heterozygosity (LOH) 1p36, DNA di/tetraploidy) were observed in 14% of 76 biologically examined cases. The median follow-up time of all the patients was 21.5 months (range 1-101 months). To date, 69 patients are in complete remission (CR) and 2 patients have died due to therapy (stage 4, 1 patient; stage 3, 1 patient with unfavourable markers). Apart from screened patients, 16 other patients with NB were found who had previously had a normal screening test, i.e. 'false negative' patients (age range 10-41 months, median 31.5 months). The median interval between screening and diagnosis was 24.5 months (range 6-35 months). 11 of the 'false negative' patients suffered from generalised NB (stage 4) and 5 had localised NB at diagnosis. Unfavourable biological markers were observed in 7/12 patients. 5 patients have died, 2 achieved partial remission and 9 CR. 9 of the 11 patients with unfavourable biological markers diagnosed due to NB screening are currently in CR. It is very likely that, among the patients without unfavourable biological markers, we detected tumours which may have regressed spontaneously. These children may have undergone 'unnecessary,' but unavoidable, diagnostic procedures and therapy. To reduce the number of 'false negative' patients, a later screening could be helpful and should be evaluated.

AB - Between January 1986 and May 1996, 870,313 children were tested in European neuroblastoma (NB) screening programmes. Among these children, 82 cases of NB (age range 4-24 months, median 11 months) were detected by screening. 83% of the patients had localised NB and 17% were diagnosed with generalised NB (stage 4, 10%; stage 4s, 7%). Unfavourable biological markers (MYCN amplification, loss of heterozygosity (LOH) 1p36, DNA di/tetraploidy) were observed in 14% of 76 biologically examined cases. The median follow-up time of all the patients was 21.5 months (range 1-101 months). To date, 69 patients are in complete remission (CR) and 2 patients have died due to therapy (stage 4, 1 patient; stage 3, 1 patient with unfavourable markers). Apart from screened patients, 16 other patients with NB were found who had previously had a normal screening test, i.e. 'false negative' patients (age range 10-41 months, median 31.5 months). The median interval between screening and diagnosis was 24.5 months (range 6-35 months). 11 of the 'false negative' patients suffered from generalised NB (stage 4) and 5 had localised NB at diagnosis. Unfavourable biological markers were observed in 7/12 patients. 5 patients have died, 2 achieved partial remission and 9 CR. 9 of the 11 patients with unfavourable biological markers diagnosed due to NB screening are currently in CR. It is very likely that, among the patients without unfavourable biological markers, we detected tumours which may have regressed spontaneously. These children may have undergone 'unnecessary,' but unavoidable, diagnostic procedures and therapy. To reduce the number of 'false negative' patients, a later screening could be helpful and should be evaluated.

M3 - SCORING: Zeitschriftenaufsatz

VL - 34

SP - 1391

EP - 1397

JO - EUR J CANCER

JF - EUR J CANCER

SN - 0959-8049

IS - 9

M1 - 9

ER -