Bone turnover biomarkers reflect radiation-induced bone injuries in women with non-metastatic rectal cancer

Author:

Magnusson Per1ORCID,Sääf Maria2ORCID,Martling Anna23ORCID,Svanström Röjvall Annika24ORCID,Atanasova Diana1ORCID,Wilamowski Franciszek5,Flöter Rådestad Angelique67ORCID,Buchli Christian23ORCID,Segelman Josefin28ORCID

Affiliation:

1. Linköping University Department of Clinical Chemistry, and Department of Biomedical and Clinical Sciences, , Linköping, SE-581 85 , Sweden

2. Karolinska Institutet Department of Molecular Medicine and Surgery, , Stockholm, SE-171 77 , Sweden

3. Karolinska University Hospital Department of Pelvic Cancer, Unit of Gastrointestinal Oncology and Colorectal Surgery, , Stockholm, SE-171 76 , Sweden

4. Capio S:t Göran’s Hospital Department of Surgery and Oncology, Unit of Gastrointestinal Oncology, , Stockholm, SE-112 81 , Sweden

5. Ersta Hospital Department of Radiology, , Stockholm, SE-116 91 , Sweden

6. Karolinska University Hospital Department of Hereditary Cancer, , Stockholm, SE-171 76 , Sweden

7. Karolinska Institutet Department of Women’s and Children’s Health, , Stockholm, SE-171 77 , Sweden

8. Ersta Hospital Department of Surgery, , Stockholm, SE-116 91 , Sweden

Abstract

Abstract Preoperative radiotherapy (RT) for non-metastatic rectal cancer reduces local recurrence rates but can cause pelvic insufficiency fractures. Despite the high morbidity from RT-induced skeletal injuries, predictive and preventive measures are lacking. How these injuries are reflected by bone biomarkers are largely unknown. The aim was to assess longitudinal changes in bone biomarkers and their relation to RT-related bone injuries in women with rectal cancer. This longitudinal cohort study includes 47 women with non-metastatic rectal cancer treated with surgery ± preoperative RT with or without chemotherapy. Sclerostin, bioactive sclerostin, C-terminal telopeptide cross-links of collagen type I (CTX), bone-specific alkaline phosphatase (BALP), and type I procollagen intact N-terminal propeptide (PINP) were measured at baseline, after RT, and 1 yr postoperatively. Pelvic magnetic resonance imaging was used for detection of skeletal injury. Sixteen of 36 (44%) irradiated women had radiation-induced bone injuries and were compared to 11 women (RT–) and 20 women (RT+) without bone injuries. Serum CTX, BALP, and PINP increased during the first year after RT in women with radiation-induced bone injuries. The difference in mean change of CTX (p=.037) and BALP (p=.042) was conferred by longitudinal regression analyses adjusted for serum estradiol. Serum sclerostin and bioactive sclerostin remained stable over time. Taken together, bone markers may be of interest for future research on fracture prediction or preventive measures in women susceptible to radiation-induced bone injury. Due to few measure points, the full pattern cannot be captured regarding the relation over time between bone biomarkers and skeletal injury from irradiation.

Funder

Swedish Cancer Society

Stockholm Cancer Society

Bengt Ihre Research Fellowship

Bengt Ihre Foundation

ALF

Stockholm County Council

Karolinska Institutet

Region Östergötland

Publisher

Oxford University Press (OUP)

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