Treatment options for thalassemia patients with osteoporosis
A N N A L S O F T H E N E W Y O R K A C A D E M Y O F S C I E N C E SIssue: Cooley’s Anemia: Ninth Symposium
Treatment options for thalassemia patients with osteoporosis
Evangelos Terpos1 and Ersi Voskaridou21Department of Clinical Therapeutics, University of Athens School of Medicine, Athens, Greece. 2Thalassemia Center, LaikonGeneral Hospital, Athens, Greece
Address for correspondence: Evangelos Terpos, Department of Clinical Therapeutics, University of Athens School ofMedicine, Alexandra General Hospital, 80 Vas. Sofias Avenue, 11528 Athens, Greece. eterpos@hotmail.com
Osteoporosis represents a prominent cause of morbidity in patients with thalassemia. The delay in sexual maturation, the presence of diabetes and hypothyroidism, the parathyroid gland dysfunction, the progressive marrow expansion, the iron toxicity on osteoblasts, the iron chelators, and the deficiency of growth hormone or insulin growth factors have been identified as major causes of osteoporosis in thalassemia. Adequate hormonal replacement, effective iron chelation, improvement of hemoglobin levels, calcium and vitamin D administration, physical activity, and smoking cessation are the main to-date measures for the management of the disease. During the last decade, novel pathogenetic data suggest that the reduced osteoblastic activity, which is believed to be the basic mechanism of bone loss in thalassemia, is accompanied by a comparable or even greater increase in bone resorption. Therefore, the role of bisphosphonates, potent inhibitors of osteoclast activation, arises as a major factor in the management of osteoporosis in thalassemia patients. Keywords: thalassemia; osteoporosis; bisphosphonates; therapy; pathogenesis Introduction
dysfunction, the accelerated hemopoiesis with pro-gressive marrow expansion, the direct iron toxicity
Thalassemia major (TM) is a hereditary hemolytic
on osteoblasts and the deficiency of growth hor-
anemia caused by a defect in the ability of erythrob-
mone (GH) or insulin growth factor I (IGF-I) have
lasts to synthesize the  chain of adult hemoglobin.
been indicated as possible causes for thalassemia-
Several bone abnormalities are present in patients
induced osteoporosis.1–3 Furthermore, iron chela-
with TM, including the enlargement of the cranial
tion has correlated with growth failure and bone
and facial bones, spinal deformities, scoliosis, nerve
abnormalities, and high desferrioxamine dosage has
compression, spontaneous fractures, and bone loss.
been associated with cartilage alterations.4,5 More
The incidence of osteopenia or osteoporosis in well-
puzzling, however, is the observation that, despite
treated TM patients has been found to be approx-
the normalization of hemoglobin levels, adequate
imately 40–50%, and therefore osteoporosis repre-
hormone replacement, and effective iron chela-
sents a prominent cause of morbidity in TM patients
tion, patients continue to show an unbalanced bone
of both genders.1 The pathogenesis of osteoporo-
turnover with an increased resorptive phase result-
sis in TM is very complicated and differs from the
ing in seriously diminished bone mineral density
pathogenesis of bone deformities characteristically
found in nontransfused patients (thalassemia inter-media; TI), who develop bone distortion mainly due
Pathogenesis of osteoporosis in
to accelerated hemopoiesis and progressive marrow
thalassemia
expansion. Several genetic and acquired factors areimplicated in bone destruction in TM. The typi-
According to the Word Health Organization, os-
cal delay in sexual maturation, the presence of di-
teoporosis is a disease characterized by low bone
abetes and hypothyroidism, the parathyroid gland
mass and microarchitectural deterioration of bone
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
tissue, leading to enhanced bone fragility and a
are needed to exact final conclusion for the associa-
consequential increase in fracture risk.8 The cut-off
tion between gene polymorphisms and bone mass in
of 2.5 standard deviations below the normal mean
TM patients, COLIA 1 gene polymorphisms seem to
in BMD for the respective age is used for the defini-
be of importance in the pathogenesis of thalassemia-
tion of osteoporosis, whereas the decrease of BMD
between 1.5 and 2.5 standard deviations below thenormal mean for the respective age is defined as
osteopenia.9 The most important factors that are
Endocrine complications. Hypothyroidism, hy-
implicated in the pathogenesis of bone loss in tha-
poparathyroidism, diabetes mellitus, and mainly
lassemia patients are described later.
hypogonadism (as delayed puberty and/or sec-ondary hypogonadism) are considered as ma-
jor causes of osteopenia/osteoporosis in TM.1–3,5
Genetic factors seem to play a role in the develop-
Hemosiderosis of the pituitary gonadotrophic cells
ment of low bone mass and osteoporotic fractures.
and iron deposition in the testes and ovaries are in-
These factors have been implicated in the pathogen-
volved in the pathogenesis of endocrine complica-
esis of postmenopausal osteoporosis, as regulator
tions in TM.14 Hypogonadism is a well-recognized
genes of BMD, but have not been studied thor-
cause of osteoporosis and osteopenia not only in
oughly in thalassemia-induced osteoporosis. The
patients with TM but also in the general population
polymorphism at the Sp1 site of the collagen type Ia1
and is characterized by high bone turnover with
(COLIA 1) gene (collagen type I is the major bone
enhanced resorptive phase.15 Estrogen and proges-
matrix protein) was studied by Wonke and col-
terone appear to inhibit osteoclast activity and pro-
leagues,10 who found that approximately 30% of the
mote bone formation, whereas testosterone has a
TM patients were heterozygotes (Ss) and 4% were
direct stimulatory effect on osteoblast proliferation
homozygotes (SS) for the Sp1 polymorphism. The
and differentiation.3 IGFs play also an important
authors have concluded that male patients with TM
role in bone remodeling. Low-serum IGF levels de-
carrying the Sp1 mutation may develop severe os-
crease osteoblast proliferation and bone matrix for-
teoporosis of the spine and the hip more frequently
mation and reduce the activation of osteoclasts.16
than patients who do not carry this mutation. The
Several studies have demonstrated a positive corre-
COLIA 1 polymorphism has been associated with
lation between the BMD of the lumbar spine and the
reduced BMD in postmenopausal osteoporosis, and
IGF-I concentration.17 It is well documented that
predisposes women to osteoporotic fractures.11 The
the GH–IGF axis is defective in TM. Thalassemia
genes encoding collagen types Ia1 and Ia2 (COLIA
patients have significantly lower circulating levels
1 and COLIA 2, respectively) are also important
of IGF-I and the corresponding binding protein
candidates for the genetic regulation of BMD, as
(IGFBP-III) than normal individuals; thus, leading
mutations that affect the coding regimens of these
to increased bone resorption, decreased bone for-
genes are implicated in the pathogenesis of osteo-
mation, and finally to bone loss.18,19
genesis imperfecta and osteoarthritis.12 The studyof COLIA 1 polymorphism may help in identify-
Iron overload and desferrioxamine. Iron deposi-
ing thalassemia patients who are at higher risk to
tion in the bone impairs osteoid maturation and
develop osteoporosis and pathologic fractures.13
inhibits mineralization locally, resulting in focal os-
Other genetic factors that have been reported to
teomalakia. The mechanism by which iron overload
correlate with bone mineral damage in adult pa-
interferes in osteoid maturation and mineralization
tients with -thalassemia include the vitamin D
includes the incorporation of iron into crystals of
receptor (VDR) Bsml BB polymorphism, the loss-
calcium hydroxyapatite, which consequently affects
of-function mutations in the gene of the vitamin
the growth of hydroxyapatite crystals and reduces
D receptor, the sequence variation of 713-8delC of
the bone metabolism unit tensile strength.20 Fur-
transforming growth factor-1, the presence of re-
thermore, desferrioxamine inhibits DNA synthesis,
striction fragment length polymorphisms for the
osteoblast, and fibroblast proliferation, osteoblast
calcitonin (CT) receptor gene, estrogen receptor and
precursors differentiation, and collagen formation,
interleukin-6 gene loci.1,13 Although further studies
although enhances osteoblast apoptosis, especially
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
in patients who receive inappropriately high doses
function.26 The RANK/RANKL/OPG pathway is of
great importance for the activation and prolifera-tion of osteoclast precursors. We and others have
Bone marrow expansion. Bone marrow expan-
shown that the ratio of sRANKL/OPG in the serum
sion, which is a typical finding in patients with
was increased in thalassemia patients with osteope-
TM, has been considered as a major cause of bone
nia/osteoporosis, providing evidence for the role of
destruction.20 Transferrin receptor studies have
RANKL/OPG system in the pathogenesis of osteo-
demonstrated increased bone marrow activity even
porosis in thalassemia.26–28 Serum levels of IL-1␣,
in patients with low reticulocyte count or marrow
TNF-␣, IL-6, and TGF-, that are able to increase
hypoplasia.22 However, there was found no direct
osteoclast function, were elevated in TM and cor-
correlation between serum levels of soluble trans-
related with bone resorption and lumbar BMD,29
ferrin receptor and the severity of osteoporosis.10
suggesting their involvement in the pathogenesis of
Vitamin deficiencies. Vitamin C deficiency in iron-
TM osteoporosis and supporting the role of the im-
overload patients with low levels of serum ascorbic
acid induces the risk of osteoporotic fractures.23 Vi-tamin D deficiency is also implicated in the patho-
Reduced osteoblast function in thalassemic pa-
genesis of osteoporosis in TM patients due to the
tients with osteoporosis. There is evidence of re-
regulatory effect of vitamin D in both osteoclasts
duced osteoblast function in TM. Histomorphom-
and osteoblasts. Adequate calcium intake and small
etry studies have revealed that increased osteoid
amounts of vitamin D administration during skele-
thickness, increased osteoid maturation and min-
ton development can increase bone mass in adoles-
eralization lag time, which indicate impaired bone
cents and decrease bone loss in adult life. However,
matrix maturation, and defective mineralization is
most studies have failed to show reduced serum lev-
present in children and adolescents with TM.20 In
els of 25-hydroxyvitamin D in TM patients.
addition, iron deposits appeared along mineral-ization fronts and osteoid surfaces, whereas focal
Physical activity. Patients with TM have reduced
thickened osteoid seams were found together with
physical activity due to the complications of the
focal iron deposits.20,30 Finally, dynamic bone for-
disease and the overprotection by their parents who
mation histomorphometry studies established re-
do not encourage muscle activity. Thus, the lack of
duced bone formation rate in TM patients.20 This
physical activity is another predisposing factor for
reduced bone formation is thought to-date to be
osteoporosis in TM patients and muscle activity has
mainly the result of iron poisoning in osteoblasts
and/or the result of reduced function of GH
These factors can lead to the destruction of bone
and IGF-1 axis in TM patients.1 However, novel
in thalassemia patients by increasing the osteoclast
molecules seem to be implicated in osteoblast dys-
function and/or reducing the osteoblast activity.
function in TM. Dickkopf-1 (Dkk-1) is a Wnt sig-
Increased osteoclast function in thalassemic pa-
naling inhibitor, which inhibits the osteoblast differ-
tients with osteoporosis. During the last decade,
entiation and function. We have recently shown that
there was sufficient data supporting that increased
serum levels of Dkk-1 were increased in TM patients
osteoclast activation is present in TM patients.
with osteoporosis and correlated with lumbar spine
Patients with TM and osteoporosis have elevated
and wrist BMD. Interestingly, when zoledronic acid
markers of bone resorption, such as N-terminal
(ZA) was given in these patients there was a reduc-
cross-linking telopeptide of collagen type-I (NTX)
tion in Dkk-1 levels, which was not observed in the
and tartrate-resistant acid phosphatase type 5b
placebo group of this randomized trial.31
(TRACP-5b)24,25 that correlated with BMD of the
Management of thalassemia-associated
lumbar spine in these patients.25,26 This increased
osteoporosis
osteoclast activity seems to be at least partially dueto an imbalance in the receptor–activator of nuclear
Prevention and general principles. Prevention
factor-kappa B ligand (RANKL)/osteoprotegerin
and treatment of early bone loss make the best pol-
(OPG) system and the overproduction of cytokines
icy. Annual checking of BMD starting in adoles-
that are involved in the osteoclast differentiation and
cence is considered indispensable. Physical activity
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
must always be encouraged. Moderate and high
Bisphosphonates. The increased bone resorption
impact activities are to be supported. Exercise has
observed in patients with thalassemia-induced os-
additional benefits: it improves cardiovascular sys-
teoporosis has led to the use of bisphosphonates in
tem, reduces the risk of diabetes, and prevents de-
the management of osteoporosis in this cohort of
pression. Smoking should be discouraged. Adequate
patients. Bisphosphonates are potent inhibitors of
calcium intake during skeleton development can
osteoclastic bone resorption. They act by inhibiting
increase bone mass in adult life and in combina-
osteoclastic recruitment and maturation, prevent-
tion with administration of low doses of vitamin
ing the development of monocyte precursors into
D may prevent bone loss and fractures.32 Early di-
osteoclasts, inducing osteoclast apoptosis and inter-
agnosis and treatment of diabetes mellitus is also
rupting their attachment to the bone. In thalassemia
important, as the association between diabetes and
osteoporosis, almost all generations of bisphospho-
low bone mass in TM patients has been well docu-
nates have been used in an attempt to increase the
mented.1 Furthermore, adequate iron chelation may
BMD and improve the abnormal bone remodeling.
prevent iron toxicity in the bone and sufficient blood
Morabito and colleagues scheduled a randomized,
transfusions may inhibit uncontrolled bone marrow
placebo-controlled study to investigate the effects
of 2 years daily oral administration of alendronateor intramascular administration of clodronate on
Hormonal replacement. Prevention of hypogo-
BMD, bone turnover markers, safety, and tolera-
nadism seems to be the most effective way for pre-
bility in 25 thalassemia patients with osteoporo-
venting osteoporosis and other bone deformities
sis.37 Patients were randomized to receive placebo
in thalassemia patients.1–3,5,32 Anapliotou and col-
(eight patients) or 100 mg of clodronate, i.m., every
leagues recommended that continuous hormonal
10 days (eight patients) or 10 mg of alendronate per
replacement therapy with transdermal estrogen for
os daily (nine patients). All patients also received
females or human chorionic gonadotrophin for
500 mg of elemental calcium and 400 IU cholecal-
males improves bone density parameters.33 How-
ciferol daily. After 2 years of follow-up, the lumbar
ever, despite hormonal replacement, calcium and
spine and femoral neck BMD had decreased signif-
vitamin D administration, effective iron chelation,
icantly in the placebo group. Clodronate reduced
and normalization of hemoglobin levels, patients
bone resorption markers, deoxypyrydinoline, and
with TM continue to lose bone mass.6,7
pyrydinoline, and inhibited bone loss but it was un-
Calcitonin. Canatan and colleagues have evaluated
able to increase BMD at all studied sites. Daily treat-
the effect of calcitonin (CT), a potent inhibitor of
ment with alendronate normalized the rate of bone
osteoclasts, on bone mass in 14 patients with TM.
turnover, and resulted in a rise in BMD of the spine
One hundred IU of CT were administered, three
and the hip. This increment was statistically signif-
times a week, for 1 year in combination with daily
icant at the femoral neck, whereas at the lumbar
administration of 250 mg of calcium. At the end
spine the gain was less marked. Alendronate caused
of treatment period, bone pain had disappeared,
few adverse effects, including upper gastrointestinal
radiological findings of osteoporosis had been im-
symptoms, but no patient discontinued the study.37
proved, and the number of fractures had been de-
The ineffectiveness of clodronate was established in
creased in the treatment group but not in controls.
another randomized, placebo-controlled trial.38
CT had no important side effects.34 Both parenteral
Pamidronate, a second-generation aminobispho-
and intranasal instillations are available.
sphonate, has been given intravenously in patientswith TM and osteoporosis. First, Wonke evalu-
Hydroxyurea. Ten patients with TM were given hy-
ated the effect of 15 mg of pamidronate on BMD.
droxyurea (HU), at a dose of 1.5 g p.o. daily, in an
Pamidronate was given in a 40 min infusion, at
attempt to reduce marrow hyperplasia diagnosed by
monthly intervals. A significant improvement in
MRI. HU improved bone pain and MRI findings.35
BMD was observed in most patients.10 Our group
However, in another study, the administration of
compared the effects of two different doses of
HU for at least 2 years did not manage to show any
pamidronate, 30 mg versus 60 mg, on BMD of the
improvement of the BMD compared with patients
lumbar spine, femoral neck, and forearm and on
markers of bone remodeling and osteoclast function
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
in 26 patients with thalassemia and osteoporosis.
groups A and B and for 12 months for group C (pa-
Thirteen patients with TM and five patients with TI
tients of group C received ZA, 4 mg every 3 months,
were given pamidronate at a dose of 30 mg in a 2 h i.v.
i.v., for 12 months after their placebo 12-month ad-
infusion, once a month for 12 months; another eight
ministration). We found, interestingly, that at the
patients (four with TM and four with TI) received
36th month, patients of group B continued to show
a dose of 60 mg/month, in an attempt to explore
an increase in the BMD of all studied sites despite
whether increasing the dose of pamidronate might
the discontinuation of ZA. Furthermore, patients of
have any additional effect. Both groups included pa-
groups A and C showed a dramatic increase in BMD
tients with comparable degrees of osteoporosis and
of all studied sites compared with baseline values (P
hypogonadism. All patients were also receiving cal-
< 0.01) The increase of BMD observed in groups A
cium and vitamin D supplement prior and during
and C was accompanied by a comparable reduction
the 12-month follow-up period of the study. Ad-
in bone resorption marker CTX at the 36th month,
ministration of 30 mg of pamidronate resulted in a
which had not reported at the 12th month; on the
significant increase of the BMD of the lumbar spine
contrary in group C there was an increase in CTX
in all patients, but not the BMD of the femoral neck
at the 12th month. These observations suggest that
and the forearm. The 60 mg of pamidronate group
ZA continues to act after its discontinuation.39
showed a similarly significant increase in the BMD
In another recent study, we confirmed that the
of the lumbar spine in both transfusion-dependent
increase of erythropoietic activity in TI, which con-
and transfusion-independent patients. Administra-
tinues irrespectively of the improvement of BMD
tion of both doses of pamidronate was also followed
produced by ZA, seems to be a major cause of bone
by a clear decrease of markers of bone resorption
loss in this hemoglobinopathy. Soluble transferrin
(NTX and TRACP-5b), OPG, and osteocalcin that
receptor (sTfR) and erythropoietin (Epo) serum
was similar in patients of both treatment groups.
levels are increased in TI but we showed for the first
Furthermore, most patients complaining for severe
time in the literature that this elevation was further
bone pain at the onset of the study had a significant
increased by time, although BMD was improved by
reduction of pain after treatment period. No severe
adverse-events were reported in this study.25
All described studies confirm the effectiveness of
Zoledronic acid is the most potent third genera-
bisphosphonates in the treatment of thalassemia-
tion bisphosphonate to-date and has been found to
induced osteoporosis. Alendronate, pamidronate,
be extremely efficacious in increasing BMD in TM
and ZA seem to have the greater efficacy. How-
patients. We reported the results of a randomized,
ever, more trials must be conducted to clarify the
placebo-controlled trial of ZA in 66 thalassemia
exact role of each biphosphonate, the long-term
patients with osteoporosis. The patients were ran-
benefit and side effects as well as the effects of
domized to receive 4 mg ZA intravenously every
the combination of bisphosphonates with other ef-
fective agents, such as hormonal replacement, in
3 months (21 patients; group B), or to receive
placebo every 3 months (22 patients; group C), for
Conclusion and future perspectives
a period of 1 year. Patients of group B had a sig-nificant increase in their lumbar spine BMD, which
Thalassemia-associated osteoporosis is multifacto-
was accompanied by dramatic reductions in bone
rial and, therefore, very difficult in its management.
pain, and bone markers. Patients in placebo group
Osteoporosis is a progressive disease; thus, preven-
showed no alteration in BMD of any studied site
tion and early diagnosis are very important. Ade-
or in bone pain scores; on the contrary, they had
quate hormonal replacement, effective iron chela-
an aggravation in bone resorption. Therefore, this
tion, improvement of hemoglobin levels, calcium
study confirmed that ZA is an effective treatment
and vitamin D administration, physical activity,
for increasing BMD and reducing bone resorption
and smoking cessation are the main to-date mea-
in thalassemia-induced osteoporosis with no serious
sures for the management of the disease. However,
side effects.28 As the duration of ZA therapy had not
novel pathogenetic data suggest that the reduced
been evaluated in any trial, we followed-up our pa-
osteoblastic activity, which is believed to be the ba-
tients for 24 months after discontinuation of ZA for
sic mechanism of bone loss in TM, is accompanied
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
by a comparable or even greater increase in bone
What are the criteria by which a densitometric diagnosis
resorption. Therefore, the role of bisphosphonates
of osteoporosis can be made in males and non-Caucasians?
arises as major in the management of osteoporo-
J. Clin. Densitom. 5(Suppl.): 19–27.
10. Wonke, B., C. Jensen, J.J. Hanslip, et al. 1998. Genetic and ac-
sis in these patients. However, many aspects have
quired predisposing factors and treatment of osteoporosis in
to be clarified before the broad use of bisphospho-
thalassaemia major. J. Pediatr. Endocrinol. Metab. 11(Suppl.
nates in TM-induced osteoporosis: which one? how
long? and at what dose? The combination of bispho-
11. Uitterlinden, A.G., A.E. Weel, H. Burger, et al. 2001. Interac-
sphonates with other effective agents has also to be
tion between the vitamin D receptor gene and collagen typeI alpha 1 gene in susceptibility for fracture. J. Bone Miner.
evaluated in randomized trials. Other novel agents
Res. 16: 379–385.
that stimulate bone formation such as teriparatide, a
12. Uitterlinden, A.G., H. Burger, C.M. van Duijn, et al. 2000.
recombinant peptide fragment of parathyroid hor-
Adjacent genes, for COL2A1 and the vitamin D receptor,
mone, strontium ranelate, a second anabolic agent,
are associated with separate features of radiographic os-
that seem to prevent osteoporotic fractures in post-
teoarthritis of the knee. Arthritis Rheum. 43: 1456–1464.
13. Perrotta, S., M.D. Cappellini, F. Bertoldo, et al. 2000. Osteo-
menopausal women, are being studied but their
porosis in beta-thalassaemia major patients: analysis of the
effects in TM-induced osteoporosis remains to be
genetic background. Br. J. Haematol. 111: 461–466.
proven. Finally, antibodies against RANKL, such as
14. Berkovitch, M., T. Bistritzer, S.D. Milone, et al. 2000. Iron
denosumab, which has just been licensed by FDA
deposition in the anterior pituitary in homozygous beta-
for the treatment of postmenopausal osteoporosis,
thalassemia: MRI evaluation and correlation with gonadal function. J. Pediatr. Endocrinol. Metab. 13: 179–184.
and antibodies against Dkk-1 or against sclerostin
15. Riggs, B.L., S. Khosla & L.J. Melton III. 1998. A unitary model
may be future agents for the effective management
for involutional osteoporosis: estrogen deficiency causes
of this difficult complication of thalassemia.
both type I and type II osteoporosis in postmenopausalwomen and contributes to bone loss in aging men. J. BoneConflicts of interest Miner. Res. 13: 763–773.
16. Geusens, P.P. & S. Boonen. 2002. Osteoporosis and the
The authors have received research support and
growth hormone-insulin-like growth factor axis. Horm. Res.58(Suppl. 3): 49–55.
17. Rucker, D., S. Ezzat, A. Diamandi, et al. 2004. IGF-I and
References
testosterone levels as predictors of bone mineral density in healthy, community-dwelling men. Clin. Endocrinol. 60:
1. Voskaridou, E. & E. Terpos. 2004. New insights into the
pathophysiology and management of osteoporosis in pa-
18. Soliman, A.T., N. El Banna, M. Abdel Fattah, et al. 1998.
tients with beta thalassaemia. Br. J. Haematol. 127: 127–139.
Bone mineral density in prepubertal children with beta-
2. Garofalo, F., A. Piga, R. Lala, et al. 1998. Bone metabolism
thalassemia: correlation with growth and hormonal data.
in thalassemia. Ann. N.Y. Acad. Sci. 850: 475–478. Metabolism 47: 541–548.
3. Voskaridou, E. & E. Terpos. 2008. Pathogenesis and man-
19. Morabito, N., A. Gaudio, A. Lasco, et al. 2004. Osteopro-
agement of osteoporosis in thalassemia. Pediatr. Endocrinol.
tegerin and RANKL in the pathogenesis of thalassemia-
Rev. 6(Suppl. 1): 86–93.
induced osteoporosis: new pieces of the puzzle. J. Bone Miner.
4. Hatori, M., J. Sparkman, C.C. Teixeira, et al. 1995. Effects of
Res. 19: 722–727.
deferoximine on chondrocyte alkaline phosphatase activity:
20. Mahachoklertwattana, P., V. Srikulchayanonta, A. Chuan-
proxidant role of deferoximine in thalassemia. Calcif. Tissue
sumrit, et al. 2003. Bone histomorphometry in children and
Int. 57: 229–236.
adolescents with beta-thalassemia disease: iron-associated
5. Olivieri, N.F. 1999. The beta-thalassemias. N. Engl. J. Med.
focal osteomalacia. J. Clin. Endocrinol. Metab. 88: 3966– 341: 99–109.
6. Lasco, A., N. Morabito, A. Gaudio, et al. 2001. Effects of hor-
21. De Sanctis, V., A. Pinamonti, A. Di Palma, et al. 1996. Growth
monal replacement therapy on bone metabolism in young
and development in thalassaemia major patients with severe
adults with beta-thalassemia major. Osteoporos. Int. 12: 570–
bone lesions due to desferrioxamine. Eur. J. Pediatr. 155:
7. Carmina, E., G. Di Fede, N. Napoli, et al. 2004. Hypogo-
22. Ma, E.S., K.K. Lam, A.Y. Chan, et al. 2003. Transferrin
nadism and hormone replacement therapy on bone mass of
receptor-2 polymorphisms and iron overload in transfusion
adult women with thalassemia major. Calcif. Tissue Int. 74:
independent -thalassemia intermedia. Haematologica 88:
8. World Health Organization. 1994. Assessment of fracture
23. Michelson, J. & A. Cohen. 1988. Incidence and treatment of
risks and its application to screening for post-menopausal
fractures in thalassemia. J. Orthop. Trauma 2: 29–32.
osteoporosis. Report of a WHO Study Group. World Health
24. Voskaridou, E., M.C. Kyrtsonis, E. Terpos, et al. 2001. Bone
Organ. Tech. Rep. Ser. 843: 1–129.
resorption is increased in young adults with thalassaemia
9. Binkley, N.C., P. Schmeer, R.D. Wasnich & L. Lenchik. 2002.
major. Br. J. Haematol. 112: 36–41.
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
25. Voskaridou, E., E. Terpos, G. Spina, et al. 2003. Pamidronate
33. Anapliotou, M.L., I.T. Kastanias, P. Psara, et al. 1995. The
is an effective treatment for osteoporosis in patients with
contribution of hypogonadism to the development of osteo-
beta-thalassaemia. Br. J. Haematol. 123: 730–737.
porosis in thalassaemia major: new therapeutic approaches.
26. Dresner Pollack, R., E. Rachmilewitz, A. Blumenfeld, et al. Clin. Endocrinol. 42: 279–287.
2000. Bone mineral metabolism in adults with beta-
34. Canatan, D., N. Akar & A. Arcasoy. 1995. Effects of calcitonin
thalassaemia major and intermedia. Br. J. Haematol. 111:
therapy on osteoporosis in patients with thalassemia. ActaHaematol. 93: 20–24.
27. Voskaridou, E. & E. Terpos. 2005. Osteoprotegerin to sol-
35. Angastiniotis, M., N. Pavlides, K. Aristidou, et al. 1998. Bone
uble receptor activator of nuclear factor kappa-B ligand
pain in thalassaemia: assessment of DEXA and MRI findings.
ratio is reduced in patients with thalassaemia-related osteo-
J. Pediatr. Endocrinol. Metab. 11(Suppl. 3): 779–784.
porosis who receive vitamin D3. Eur. J. Haematol. 74: 359–
36. Kosaryan, M., M.F. Zadeh & V.K. Shahi. 2004. The bone
density of thalassemic patients of Boo Ali Sina hospital, Sari,
28. Voskaridou, E., A. Anagnostopoulos, K. Konstantopoulos,
Iran in 2002; does hydroxyurea help? Pediatr. Endocrinol.et al. 2006. Zoledronic acid for the treatment of osteoporo-
Rev. 2(Suppl. 2): 303–306.
sis in patients with beta-thalassemia: results from a single-
37. Morabito, N., A. Lasco, A. Gaudio, et al. 2002. Bisphospho-
center, randomized, placebo-controlled trial. Haematologica
nates in the treatment of thalassemia-induced osteoporosis. 91: 1193–1202. Osteoporos. Int. 13: 644–649.
29. Morabito, N., G.T. Russo, A. Gaudio, et al. 2007. The “lively”
38. Pennisi, P., G. Pizzarelli, M. Spina, et al. 2003. Quantitative
cytokines network in beta-Thalassemia Major-related osteo-
ultrasound of bone and clodronate effects in thalassemia-
porosis. Bone 40: 1588–1594.
induced osteoporosis. J. Bone Miner. Metab. 21: 402–408.
39. Voskaridou, E., D. Christoulas, M. Konstantinidou, et al.
Angchaisuksiri, et al. 2003. Abnormalities in bone
2008. Continuous improvement of bone mineral density
mineral density and bone histology in thalassemia. J. Bone
two years post zoledronic acid discontinuation in patients
Miner. Res. 18: 1682–1688.
with thalassemia-induced osteoporosis: long term follow up
31. Voskaridou, E., D. Christoulas, C. Xirakia, et al. 2009. Serum
a randomized, placebo-controlled trial. Haematologica 93:
Dickkopf-1 is increased and correlates with reduced bone
mineral density in patients with thalassemia-induced os-
40. Voskaridou, E., D. Christoulas, E. Antoniadou & E. Terpos.
teoporosis. Reduction post-zoledronic acid administration.
2008. Continuous increase in erythropoietic activity despite
Haematologica 94: 725–728.
the improvement in bone mineral density by zoledronic
32. Lindsay, R. 1993. Prevention and treatment of osteoporosis.
acid in patients with thalassemia induced osteoporosis. ActaLancet 341: 801–805. Haematol. 119: 40–44.
Ann. N.Y. Acad. Sci. 1202 (2010) 237–243 c 2010 New York Academy of Sciences.
FICHA DE DATOS DE SEGURIDAD R.D. 255/2003 SEGÚN 2001/58/CE________________________________________________________________________________________________________________________________________________________________________________________________________________________01.02 Uso: Neutralizante de alcalinidad y restos de oxidantes (cloro)____________________________________________________
Maryland Early Brass Festival Elisa Koehler, Director Evening Concert Featuring Brian Shaw, Baroque Trumpet The festival gratefully acknowledges support from the Laura Graham Cooper Lecture Fund. Opening Fanfare and Words of Welcome Aire de Trompete Georg Philipp Telemann (1681-1767) Sonata in D Major Henry Purcell (c. 1659-1695) Sonata in D for Two Trumpets Petronio Fra