CHAPTER IV

1. CHAPTER IV Other osteopathies

2. Other osteopathies 57 New susceptibility loci in Paget’s disease of bone • The presence of sequestosome mutations in familial or sporadic formes of Paget ‘s disease is well known • Results of a large genomic study • Loci other than the sequestosome (SQSTM1) ? • 750 patients with Paget’s disease (without SQSTM1 mutation) • 2 699 control • Replicated data in 500 patients with Paget’s disease and 535 controls Sporadic forms Familiar forms 60 40 % 40 Patients with the SQSTM1 mjutation (%) 20 11 % 0 • M-CSF, DC-STAMP, RANK: key role in osteoclast differentiation • Optineurin function not yet elucidated • This study identifies 4 new susceptibility loci and reinforces the interest of the genetic approach for the comprehension of Paget’s bone disease pathogeny ASBMR 2010 - D’après Albagha O et al., Édimbourg, Royaume-Uni, abstr. 1031, actualisé

3. Crossbreed of TRAP-MVP mice (expressing the nucleocapsid of measles virus) and developing morphological anomalies in osteoclasts (OC), with p62P394-Ki mutated mice, carriers of a SQSTM1 mutation that develops only functional anomalies of OC [hypersensibility to RANK and 1,25(OH)2D] Results Association of the mutation of SQSTM1 with nucleocapsid of the measles virus produces pagetoid localized lesions in mice Other osteopathies 58 Paget’s disease: role of the sequestosome mutation and of measles virus. Towards a murin model ? The p62KI/MVNP mice develop pagetoid bone lesions Controls p62KI/MVNP ( TRAP Coloration) • this model seems to reconciliate the genetic and viral hypothesis… ASBMR 2010 - D’après Kurihara N et al., Pittsburgh, États-Unis, abstr. 1032 actualisé

4. Other osteopathies 59 Circulating osteogenic cells and nonhereditary heterotopic periarticular ossification (NHPO) • Circulant osteogenic precursors (COP), derived from the bone marrow, associated with heterotopic ossifications of the progressive ossifying fibrodysplasia • The authors demonstrate that the COP contribute also to the formation of periarticular NHPO after CNS injury, medullary trauma, cranial trauma and after arthoplasty • immunohistochemistry study of postchirurgical bone pieces: coexpression of type I collagen and of CD45 • association between the COP and early fibroproliferative and neovascular stages of OH • MO/COP in the regions without HO( heterotopic ossification) Formation stages of OHNH Extraskeletic soft tissue Lymphocytic perivascular Infiltration Soft tissue Infiltration Fibroproliferation Injury Heterotopic bone Coll I CD45 Damaged tissue release Early stages Endochondral bone formation CXCR4 Mature bone Cartilage formation Neovascularization COP osteogenic precursors Inflammatory cytokines migration (SDF-1, BMP4) Étapes tardives ASBMR 2010 - D’après Egan K et al., Philadelphie, États-Unis, abstr. 1013, actualisé

5. 7 patients XLH and 6 controls Discontinuation of all therapies 2 weeks before the study 200 UI of salmon calcitonin intradermal Dosages of serum levels of GF-23, phosphatemia, calcemia, PTH, 1,25(OH)2 D3 for the following 26 hours Other osteopathies 60 Serum levels of FGF-23 after calcitonin (CT) injection in carriers of X-linked hypophosphatemia (XLH) 75 150 55 125 FGF-23 (pg/ml) Phosphatemia change (%) 100 35 75 15 50 -2 4 10 18 21 24 26 -2 4 10 18 21 24 26 Duration (hours) Duration (hours) 200 150 175 130 150 Changes in 1,25 (OH)2D3 (%) Changes in PTH(%) 110 125 90 100 70 75 -2 4 10 18 21 24 26 -2 4 10 18 21 24 26 Duration (hours) Duration (hours) • CT injection reduces rapidly serum levels of FGF/23 ; this reduction will be maintained for 16 hours. No FGF/23 modification in the control group • Comparable increase of 1.25 (OH)2 D3 levels in the 2 groups • Significant increase of phosphatemia and of TmP/GFR in the XLH group • CT : future treatment for XLH ? ASBMR 2010 - D’après Liu E et al., New Haven, États-Unis, abstr. FR0146, actualisé

6. Before traitement 12 weeks Other osteopathies 61 A promising enzymatic treatment for hypophosphatasia • Hypophosphatasia:  activity of TNSALP (Tissue-Non Specific Alkalin Phosphatase) • accumulation of inorganic pyrophosphate , mineralization inhibitor • rickets • Open label, phase II study • ENB-0040: human recombinant fusion proteinof TNSALP • 13 children (2 boys, 11 girls, 5-12 years) • 2 to 3 mg/kg s.c. 3 x /week for 24 weeks • At 6 months • Treatment well tolerated •  alkaline phosphatase activity • Absence of hypocalcemia (no "hungry bone") •  disease markers (PPi, PLP) • Improvement of radiographic aspects • motricity, force, and agility improvement •  of pain and disability Serum alkaline phosphatase 16 000 14 000 12 000 10 000 8 000 U/l 5 613 5 493 5 253 4 338 6 000 4 000 2 000 45 0 Initial level w6 w12 w18 w24 • The ENB-0040 is a promising treatment for hypophosphatasia in children ASBMR 2010 - D’après Greenberg CR et al., Saint-Louis, États-Unis, abstr. 1016, actualisé

7. Other osteopathies 62 Use of teriparatide in severe periodontitis • Objective: to evaluate the effect of teriparatide (PTH1-34), in addition to periodontal surgery, in patients with severe periodontitis • Randomized, monocenter, double-blind, placebo-controlled study • 40 patients without osteoporosis: surgery • 20 (9 ♂,11 ♀, 48 years [30-61]): + PTH1-34 20 µg/j injection + 1 g calcium and 800 UI vit. D/j for six weeks • 20 (6 ♂,14 ♀, 57 years [31-65]): + placebo injection+ 1 g calcium and 800 UI vit. D/j for six weeks • Follow-up: 12 months 1,86 mm+ 0,31 mm 2,42 mm+ 0,33 mm 1,58 mm+ 0,42 mm 2,4 2,5 3,2 Teriparatide 2,8 2,0 Teriparatide 2,0 Teriparatide 2,4 1,6 1,5 Bone gain (mm) 1,32 mm+ 0,37 mm 2,0 1,2 1,0 Reattachment level gain (mm) Periodontal pocket depth reduction (mm) 0,42 mm+ 0,29 mm 0,16 mm+ 0,24 mm 1,6 Placebo 0,8 Placebo 0,5 1,2 Placebo 0,4 0,8 0 Month 0 Month Month 0 0 0 3 6 1,5 3 6 0 1,5 3 6 9 12 9 12 9 12 • 6-week of teriparatide treatment combined with surgical treatment improves the clinical and radiological parameters of periodontitis at 12 months ASBMR 2010 - D’après Bashutski (1018)

8. Other osteopathies 63 Treatment of mammary bone metastasis in rats with anti-IL-6R (tocilizumab) antibodies Osteolysis MR16-1 +tocilizumab 2,5 Tocilizumab Placebo MR16-1 2 1,5 MR16-1 +tocilizumab Jour 21 Tocilizumab Placebo MR16-1 Surface of the cortical bone (mm²) 1 0,5 0 Tumoral bud 7 Jour 21 6 5 T : tumor BM : bone marrow 4 Tumoral surface (mm²) 3 2 1 • Antibody anti-IL-6R treatment results in a reduction of the osteolysis and in a reduction of the tumor progression • IL-6 is a potential target in breast cancer treatment 0 Placebo Tocilizumab MR16-1 + tocilizumab MR16-1 ASBMR 2010 - D’après Boernert K et al., Sydney, Australie, abstr. FR0133, actualisé

9. Other osteopathies 64 Activation of Notch pathway and osteosarcomas Notch pathway Osteomas Osteosarcomas Nucleus Delta, Jagged Notch PS1, PS2 Control NICD • Telangiectasias • Osteoid tumor • Osteoblastic cells wrongly differentiated • Necrosis • Hemorrhage MAML NICD BRJK Nucleus • Permanent activation of the Notch pathway is rapidly accompanied by the emergence of multiple osteomas • Old animals develop osteosarcomas • Notch represents a new therapeutic target for osteosarcomas ASBMR 2010 - D’après Tao J et al., Houston, États-Unis, abstr. FR0135, actualisé

10. Prerequisites adiponectin (ADPN) deficient mices have a more agressive form of multiple myeloma evolution of patients with a MGUS and a low level of ADPN tends more towards a MM than patients with more elevated ADPN levels  ADPN induces the apoptosis of myeloma cells Objective: effect of increased ADPN levels on the development of MM in vivo Design: 4-week treatment of C57Bl/KaLwRij mice with L-4F, ADPN mimetic peptide , then inoculation of 5TGM1 myeloma cells.. L-4F is maintained through the end of experiment Other osteopathies 65 Role of adiponectin in myelomas Placebo L-4F 12 Number of lytic lesions 100 10 *p < 0,01 versus placebo 25 p < 0,001 8 Placebo 20 Serum concentration in IgG2b (mg/ml) 6 15 * 50 Survival (%) 10 4 L-4F 5 * 2 0 p < 0,0001 L-4F Placebo 0 0 0 10 20 30 0 10 20 30 Days • In vitro, L-4F has not a direct effect on myeloma cell growth but directly induces ADPN expression per stromal cell in bone marrow • This study indentifies ADPN and L-4F as potential therapeutic approaches ASBMR 2010 - D’après Fowler J et al., Nashville, États-Unis, abstr. 1085, actualisé

11. Total OPN MMP7 OPN cleavage MMproliferation MMapoptosis Other osteopathies 66 Role of metalloproteinase (MMP)-7 in myeloma • Prerequisites : elevated MMP7 level is correlated to a tumoral invasion and to survival in different types of solid cancer • Hypothesis : MMP7 increases myeloma development in vivo** • Mice myeloma C57Bl/Rag2-/- MMP7-/- ***p < 0,001 *** 300 *** ** 12 Control + MM **p <0,01 16 MMP7-/- + MM 200 12 **p < 0,01 ***p < 0,001 8 Number of bon lesions Taux sériques d’ostéopontine(ng/ml) Controls *** Serum IgG2b (mg/ml) 8 MMP7 -/- 100 4 4 ** 20 0 0 0 2 4 Controls MMP7 -/- Controls 5TGM1 MM Duration as of inoculation of myeloma cells (weeks) • Osteopontin (OPN) is increased in myelomas, with different biological functions, according to its size • The long form increases proliferation of myeloma cells • The truncated form favors apoptosis of myeloma cells • MMP7 cleaves osteopontin and would favor apoptosis of myeloma cells ASBMR 2010 - D’après Lynch C et al., Nashville, États-Unis, abstr. 1086, actualisé

12. SMO Shh Hh Gli2 PTCH1 Gli2 Act Activation Cyclin D, Cyclin E, MycGit1, Patch Gli2 Act Nucleus Cytoplasm Other osteopathies 67 Degenerative disc disease: blame the hedgehog ! Hedgehog pathway • Fundamental role of the hedgehog pathway and the Gli2 transcription factor in the spine formation 18 days 2 months Wild Gli2f/f mice Gli2-deficient miceGli2f/f; Col2CreER • After deletion of Gli2, a rapid destruction of intervertebral disc and a vertebral fusion are observed • Hedgehog pathway plays an essential role in degenerative disc disease ASBMR 2010 - D’après Zeng F et al., Rochester, États-Unis, abstr. 1121, actualisé