BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE

M. Macnicol; P. Crofton; C. Macfarlane; B Wardhaugh; M. Ranke

doi:10.1302/0301-620X.85BSUPP_III.0850259c

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BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE

M. Macnicol
P. Crofton
C. Macfarlane
B Wardhaugh
M. Ranke

BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE

Macnicol M, Crofton P, Macfarlane C, Wardhaugh B, Ranke M. BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE. Orthop Procs. 2003;85-B(SUPP_III):259-260. doi:10.1302/0301-620X.85BSUPP_III.0850259c

Macnicol, M., et al. “BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE.” Orthopaedic Proceedings, vol. 85-B, no. SUPP_III, 2003, pp. 259-260., https://doi.org/10.1302/0301-620X.85BSUPP_III.0850259c

Macnicol, M., Crofton, P., Macfarlane, C., Wardhaugh, B., & Ranke, M. (2003). BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE. Orthopaedic Proceedings, 85-B(SUPP_III), 259-260. https://doi.org/10.1302/0301-620X.85BSUPP_III.0850259c

Macnicol, M., Crofton, P., Macfarlane, C., Wardhaugh, B. and Ranke, M. (2003) “BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE.” Orthopaedic Proceedings, 85-B(SUPP_III), pp. 259-260. Available at: https://doi.org/10.1302/0301-620X.85BSUPP_III.0850259c

Macnicol, M., P. Crofton, C. Macfarlane, B Wardhaugh, and M. Ranke. “BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE.” Orthopaedic Proceedings 85-B, no. SUPP_III (2003): 259-260. https://doi.org/10.1302/0301-620X.85BSUPP_III.0850259c

Macnicol M, Crofton P, Macfarlane C, Wardhaugh B, Ranke M. BONE TURNOVER AND GROWTH IN CHILDREN FOLLOWING ACUTE ONST OF PERTHES DISEASE. Orthop Procs. 2003 Mar 1;85-B(SUPP_III):259-260. https://doi.org/10.1302/0301-620X.85BSUPP_III.0850259c

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Abstract

Objectives: (1) To establish whether the acute phase of Perthes’ disease is associated with abnormalities of growth or bone/collagen turnover. (2) To investigate subsequent changes during treatment and healing.

Methods: In a longitudinal study of 9 children (7 boys), mean age 6.5years (range 3.0 -9.8 years), we serially monitored insulin-like growth factor (IGF)-I, IGF binding protein (BP)-3, bone alkaline phosphatase (ALP, osteoblast activity), C-terminal propeptide of type I collagen (PICP, bone collagen synthesis), C-terminal telopeptide of type I collagen (ICTP, bone collagen degradation), and N-terminal propeptide of type III collagen (P3NP, soft tissue collagen synthesis) in weeks 1,2 and 12 following acute presentation with a limp and again (in 7/9 patients) 1-2 years after presentation. We measured lengths of both lower legs by knemometry at weeks 1,2,6 and 12. Height and weight were measured at baseline and at year 2 follow-up.

Results: Stature was normal at presentation but height SD score subsequently declined (P: 0;06). In week 1, patients already had low circulating IGF-I (P < 0.05), PICP and P3NP (P < 0.0001) and increased ICTP (P:0.001) compared with age ang sex-matched reference groups, indicating low rates of collagen synthesis and enhanced rates of collagen breakdown. Normal or high body mass index ruled out under-nutrition as a cause for the low IGF-I. IGF-I, ICTP and P3NP showed little further change over the next 2 years. Increases in bone ALP and PICP during follow-up (P < 0.06) may have reflected healing of infarcted epiphysis or increased bone turnover associated with reduced physical activity. Year 2 height SD scores correlated with IGF-I (r +0.83, P < 0.05), suggesting that persistently low IGF-I may have contributed to declining height SD scores. Asymmetrical lower leg growth observed during the acute phase may reflect differential weight-bearing on affected and unaffected limbs. Subsequent cessation, then resumption of symmetrical lower leg growth probably reflected our treatment of immobilisation followed by gentle remobilisation.

Conclusions: This study provides insights into the patho-physiology of the growth abnormalities associated with the fragmentation and healing phases of Perthes’ disease.

Local Host: British Society for Children’s Orthopaedic Surgery. Conference Theme: Congenital Deficiencies of the Lower Limb. These abstracts were prepared by A.Catterall.