Hindawi Publishing Corporation
Journal of Osteoporosis
Volume 2012, Article ID 162806, 8 pages
doi:10.1155/2012/162806

Research Article

Detecting Early Biomechanical Effects of Zoledronic Acid
on Femurs of Osteoporotic Female Rats

Evandro Pereira Palacio,1 Sérgio Swain Müller,2 Trajano Sardenberg,2

Roberto Ryuiti Mizobuchi,1 José Antônio Galbiatti,1 Alcides Durigan Jr.,1

Aniello Savarese,3 and Érika Veruska Paiva Ortolan2

1 Department of Orthopaedics and Trauma Surgery, Marilia State Medical School, FAMEMA, Marilia, SP 17519-030, Brazil
2 Department of Surgery and Orthopaedics, Botucatu Medical School, UNESP, Botucatu, SP 18618-000, Brazil
3 Department of Medical Education, Marilia State Medical School, FAMEMA, Marilia, SP 17519-030, Brazil

Correspondence should be addressed to Evandro Pereira Palacio, palacio@famema.br

Received 3 June 2012; Revised 30 September 2012; Accepted 19 October 2012

Academic Editor: Jean Jacques Body

Copyright © 2012 Evandro Pereira Palacio et al. This is an open access article distributed under the Creative Commons Attribution
License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly
cited.

Aim. To investigate the biomechanical effects of zoledronic acid (ZA) on femurs of female osteoporotic rats after follow-up periods
of 9 and 12 months. Methods. Eighty female Wistar rats were prospectively assessed. At 60 days of age, the animals were randomly
divided into two groups: bilateral oophorectomy (O) (n = 40) and sham surgery (S) (n = 40). At 90 days of age, groups O and S
were randomly subdivided into four groups, according to whether 0.1 mg/kg of ZA or distilled water (DW) was intraperitoneally
administered: OZA (n = 20), ODW (n = 20), SZA (n = 20), and SDW (n = 20). The animals were sacrificed at 9 and 12
months after the administration of the substances, and then their right femurs were removed and analyzed biomechanically. Axial
compression tests that focused on determining the maximum load (N), yield point (N), and stiffness coefficient (N/mm) of the
proximal femur were performed in the biomechanical study. Results. ZA significantly increased the maximum load and yield point,
reducing the stiffness coefficient concerning the oophorectomy status and follow-up period. Conclusion. Zoledronic acid, at a dose
of 0.1 mg/kg, significantly increased the maximum loads and yield points and reduced the stiffness coefficients in the femurs of
female rats with osteoporosis caused by bilateral oophorectomy.

1. Introduction

Osteoporosis can be considered a pandemic. Approximately
1.66 million fractures due to osteoporosis are estimated to
occur worldwide every year, and this number is expected to
quadruple by the year 2050 [1–3].

Because its insidious and silent evolution, fractures are
one of the most frequent symptoms. These fractures result
from a loss of bone mass and a fragile microscopic architec-
ture of the bone tissue. Osteoporotic fractures are associated
with a direct or indirect force on weakened bone tissue,
which induces continuity failures in the trabeculae [4–6].
Some medications, such as bisphosphonates, can stop and
even reverse the degenerative disease process in the bone.

Bisphosphonates are derived from pyrophosphate and
are used in diseases with high rates of bone remodeling, such

as Paget’s disease, bone tumors, malignant hypercalcaemia,
and osteoporosis [5, 7–9]. Given their high affinity for bone
calcium, these substances act specifically on skeletal tissue
and reduce its reabsorption by inhibiting osteoclasts. Zole-
dronic acid (ZA), a new bisphosphonate, has been shown to
be the most potent inhibitor of bone reabsorption. Studies
have shown that ZA is up to 100 times more effective than
alendronate and up to 10,000 times more effective than
etidronate, besides its once a year posology [10–13].

Several existing bisphosphonates work on the bone tissue
increasing its mass; however, there are not enough studies
that explain how those drugs act on bone mechanical
performance.

The aim of the present study was to investigate the effects
of ZA on the biomechanical properties of femoral bone tissue
in osteoporotic female rats.



2 Journal of Osteoporosis

Figure 1: Oophorectomy procedure.

2. Materials and Methods

Eighty 30-day-old female Wistar rats (Rattus norvergicus
albinus) were used. After being clinically evaluated and
weighted, they were housed in polypropylene cages with a
controlled temperature and light-dark cycle environment,
with a rodent diet (Labina, Nestlé Purina PetCare Company)
and water ad libitum.

Upon reaching a reproductive age (i.e., at 60 days of
age, which was 30 days after their arrival in the laboratory),
the rats were equally and randomly assigned in two groups:
group O (oophorectomy) (n = 40) and group S (sham
surgery) (n = 40). The random assignment was conducted
using opaque, sealed envelopes.

An oophorectomy was performed after intraperitoneal
anesthesia with 30 mg/kg of 3% sodium pentobarbital and a
bilateral dorsolateral trichotomy just below the last rib, under
sterile conditions. A longitudinal incision approximately
1.5 cm in length was made on the skin between the last
rib and the hip joint. The peritoneal cavity was exposed,
and the muscle layer was divulsed for access to the ovary
and its surrounding adipose tissue. The ovary was ligated
with a 3.0 cotton thread and resected distally to the ligature
(Figure 1). The muscle and skin were joined with a 3–0 mono
nylon suture, and the same procedures were repeated on the
contralateral side to remove the other ovary. The animals
in group S were submitted to the same procedure described
above, except for the ligation and resection of the ovaries.

A new sorting was performed at 90 days of age (30 days
after the surgical procedures), and groups O and S were
further subdivided into four subgroups according to whether
they received 0.1 mg/kg of ZA (Aclasta, Novartis Biociências
S.A.) or distilled water (DW) intraperitoneally, which yielded
the following groups: OZA (n = 20), ODW (n = 20), SZA
(n = 20), and SDW (n = 20).

Ten animals were randomly selected from each group and
sacrificed after nine or 12 months of receiving the substances
(moments 1 and 2) with a lethal intraperitoneal dose of
3% sodium pentobarbital at 80 mg/kg. The animals’ right
femurs were disarticulated at the proximal (hip) and distal
(knee) areas soaked in a 0.9% saline solution, wrapped in
aluminum foil, labeled, and stored in a freezer at a controlled
temperature of−20◦C for 24 hours until the mechanical tests
were performed.

Figure 2: Biomechanical test preparation.

Axial compression tests were performed to determine
the mechanical properties of the femurs using the Universal
Testing Machine EMIC, model DL 10,000, with an accuracy
of±(0.018 + F/3700) kN, calibrated accordingly to ISO 7500-
1:2004 and ABNT NBR 6674:1999 standards. The machine
interfaced with a computer running Windows 2000 and the
Mtest program (DDL, MN, USA), which provided graphical
control and was used to record the results.

The femurs were thawed 12 hours before the mechanical
tests and kept wrapped in gauze soaked with a 0.9% saline
solution. The distal extremities of the specimens were then
fixed (in a proportion of 2 : 3) vertically in 35 mL plastic
containers containing 30 mL of auto-polymerizing acrylic
resin. The vertical fixation of the samples was achieved with
the aid of a goniometer positioned in two orthogonal planes
with respect to the femurs.

A cleaver with a blunt concave edge (approximately
2 mm diameter), fixed to the assay machine, was manually
positioned axially to the femur and aligned with its head
(Figure 2), until the computer software indicated an axial
preload of 0,1N. Once the test was initiated, the cleaver of
the testing machine descended axially on the femoral head at
a constant speed of 30 mm/min [14–18] (Figure 3). The M
test program interrupted the test at the specimen’s breaking
point and automatically provided the results.

The maximum load (ML) (Newtons-N) upon rupture
and the load-deformation curve were automatically provided
by the program (Figure 4). The other variables, including
the yield point (YP) (Newtons-N) and stiffness coefficient
(SC) (Newtons per millimeters-N/mm), were calculated by
applying Johnson’s method to the results provided by the
program.

3. Statistical Analysis

The statistical analysis comprised a completely randomized
analysis of variance model and Tukey’s multiple comparison
tests in the SigmaStat version 3.5.1.2 (Systat Software, Inc.,
Germany, 2006) and Minitab version 15.1.30.0 (Minitab Inc.,



Journal of Osteoporosis 3

Figure 3: Bone breaking point.

208

156

104

52

0

0 1 2 3

Deformation (mm)

Load-deformation curve

St
re

n
gt

h
 m

od
u

lu
s 

(N
)

Figure 4: Load-deformation curve.

2007) statistical software. The variables were assessed using
a 2 × 2 × 2 analysis of variance factorial design with the
following three factors (each with two levels):

(i) surgical procedure (oophorectomy versus sham
surgery);

(ii) substance administered (ZA acid versus DW);

(iii) moment of euthanasia (nine versus 12 months).

Both longitudinal and cross-sectional statistical studies
were performed, in order to investigate the biomechanical
parameters and conclude if (a) there was a “time influence,”
(b) if there was a “drug influence” and (c) if there was a
“surgery influence.” A repeated measurement two-way anal-
ysis of variance (ANOVA) for the longitudinal study design
over the biomechanical parameters were used. If F values
for a given variable were found to be significant, a paired

Student’s t-test was employed. Equally, the cross-sectional
study design used a two-way ANOVA analysis. When F values
were found to be significant, a Holm-Sidak’s post hoc test was
used.

For all the comparisons, differences were deemed to be
statistically significant at P < 0.05.

4. Results

All the biomechanical measurements, averages, and P values
are displayed in Tables 1, 2, 3, and 4.

The analysis of variance revealed a significant increase in
the maximum load and yield point and a significant decrease
in the stiffness coefficient of the femurs of those animals
receiving ZA (the OZA and SZA groups), as compared to
those that received DW (the ODW and SDW groups).

A significant decrease in the maximum load and yield
point and a significant increase in the stiffness coefficient
were observed after nine months (moment 1) in the animals
that were submitted to the oophorectomy procedure and
received DW (group ODW) as compared to the nonoop-
horectomized group (group SDW). However, this difference
was no longer present at 12 months (moment 2).

The analysis of variance showed that the nonoophorec-
tomized animals that received DW (group SDW) had signif-
icantly higher maximum load and lower stiffness coefficients
at nine months (moment 1) than at twelve months (moment
2). The yield point was not affected by the moment of
euthanasia.

5. Discussion

Zoledronic acid was selected in this study due to its high
rates of positive bone balance with only one annual dose,
decreasing patients’ noncompliance with the treatment [19,
20]. The trabecular bone is the main site of action of
these drugs, preserving the thickness and density of the
bone connections and increasing the resistance of the bone
to fractures [21–23]. Patients with severe postmenopausal
osteoporosis, that have a high osteoclastic activity, may
greatly benefit from this third generation bisphosphonate,
simply by keeping their bone mass [22].

Bone tissue has the following three important mechanical
properties: bone resistance, which roughly translates to the
amount of calcium in the tissue and is defined by the
maximum load; stiffness, which represents the fragility of the
material and is defined by the stiffness coefficient; and yield
point, which is the limit at which irreversible structural dam-
age occurs without the possibility of restoring the original
shape. These properties can only be studied experimentally
by observing bone behavior when subjected to loading
forces. The equipment used in this study, which provided
highly accurate results, was developed for testing isotropic
materials (e.g., metals); however, biological materials are
viscoelastic in nature. The results obtained were not absolute,
given the limitations of the measurement techniques.

For determination of biomechanical properties, the assay
machine applied to the femurs an axial load under the



4 Journal of Osteoporosis

Table 1: Maximum load (N) at 9 and 12 months.

Group
Maximum Load

9 months 12 months

Animal Measurement (N) Mean ± SD Animal Measurement (N) Mean ± SD

ODW

1 134.5

124.2 ± 12.1

11 119.1

112.6 ± 8.9

2 111.4 12 95.4

3 105.8 13 111.5

4 110.5 14 113.1

5 133.2 15 116.8

6 137.1 16 120.5

7 135.4 17 124.2

8 125.1 18 107.5

9 115.7 19 101.7

10 133.1 20 116.3

OZA

31 128.8

141.4 ± 9.8

21 125.4

138.7 ± 9.1

32 133.2 22 131.7

33 152.5 23 147.2

34 151.7 24 149.3

35 137.0 25 133.1

36 137.4 26 135.8

37 158.4 27 153.0

38 139.0 28 140.7

39 132.8 29 129.4

40 143.0 30 141.2

SDW

41 126.0

140.0 ± 6.6

51 109.0

118.4 ± 10.5

42 138.9 52 111.0

43 149.4 53 125.5

44 135.7 54 110.3

45 141.4 55 116.8

46 136.8 56 110.6

47 147.1 57 124.1

48 144.2 58 140.9

49 138.4 59 109.7

50 142.0 60 126.3

SZA

71 142.5

149.7 ± 4.3

61 142.7

151.0 ± 9.7

72 152.9 62 150.4

73 151.7 63 154.1

74 147.1 64 148.9

75 152.8 65 137.6

76 154.9 66 170.7

77 149.2 67 150.2

78 154.2 68 140.4

79 143.7 69 158.8

80 148.5 70 156.7

speed of 30 mm/min, considered by other authors [14–18]
as the ideal average speed for viscoelastic materials (bone). It
was also taken into consideration the capacity and type of
the used assay machine, which does not allow high speed
or impact testing. Since the scope of this study was to
evaluate only fractures around the hip, the femurs were
distally fixated in the acrylic resin in a proportion of 2 : 3;
in others studies that considered fractures of the femurs at

lower sites (diaphysis and lower diaphysis fractures), femurs
were fixated in a proportion of 1 : 3 [14, 15].

The maximum load, defined as the maximum load
supportable before the breaking point, was automatically
determined by the software; it represents the highest point
in the load-deformation curve. Analyzing this variable is
essential for studying the biomechanics of any material. The
region of interest (ROI) chosen in the present study was



Journal of Osteoporosis 5

Table 2: Yield point (N) at 9 and 12 months.

Group
Yield Point

9 months 12 months

Animal Measurement (N) Mean ± SD Animal Measurement (N) Mean ± SD

ODW

1 122.8

113.0 ± 11.4

11 113.3

105.7 ± 9.0

2 110.5 12 90.8

3 120.3 13 102.4

4 97.5 14 106.3

5 117.1 15 107.6

6 97.7 16 118.1

7 118.5 17 115.2

8 123.5 18 98.6

9 97.5 19 95.4

10 125.0 20 110.6

OZA

31 127.4

129.7 ± 6.0

21 100.5

119.8 ± 9.7

32 131.8 22 111.4

33 134.2 23 124.5

34 123.5 24 130.6

35 125.1 25 119.2

36 122.5 26 119.5

37 131.8 27 134.0

38 127.5 28 122.2

39 130.4 29 112.6

40 143.2 30 123.7

SDW

41 113.5

125.3 ± 9.1

51 124.0

112.6 ± 6.2

42 119.4 52 103.7

43 118.2 53 114.1

44 119.6 54 107.3

45 131.1 55 106.5

46 133.2 56 111.6

47 135.7 57 116.2

48 129.8 58 115.2

49 137.9 59 108.3

50 114.6 60 118.1

SZA

71 133.3

137.0 ± 10.7

61 103.9

124.6 ± 16.8

72 124.4 62 128.5

73 141.0 63 111.4

74 135.8 64 126.7

75 149.5 65 120.0

76 152.0 66 152.1

77 139.8 67 110.4

78 116.1 68 128.7

79 137.2 69 112.2

80 141.7 70 152.3

the proximal femur, which is a region that is greatly affected
by osteoporosis due to the high concentration of trabecular
bone. The significantly increased maximum load in the
ZA groups (OZA and SZA) can probably be explained by
inhibition of osteoclast activity, which diminished the osteo-
porotic process even in the oophorectomized group (OZA).
In similar biomechanical investigations [14, 15], compressive
tests conducted on bone regions with lower concentrations

of trabecular bone, such as the tibial diaphysis, produced
nonsignificant results. The hormonal deficit caused by a
bilateral oophorectomy results in a loss of bone mass and
consequent decrease in the maximum load. The animals
in the present study that received ZA (the OZA group),
even those subjected to oophorectomy, had maximum loads
equivalent to those of the nonoophorectomized group (the
SZA group).



6 Journal of Osteoporosis

Table 3: Stiffness coefficient (N/mm) at 9 and 12 months.

Group
Stiffness Coefficient

9 months 12 months

Animal Measurement (N/mm) Mean ± SD Animal Measurement (N/mm) Mean ± SD

ODW

1 207.4

214.2 ± 19.0

11 218.4

236.2 ± 24.4

2 201.0 12 272.4

3 198.8 13 209.8

4 219.2 14 235.6

5 257.1 15 273.0

6 211.6 16 222.5

7 190.7 17 201.7

8 225.9 18 236.9

9 203.8 19 254.2

10 226.5 20 237.5

OZA

31 160.2

158.2 ± 9.1

21 175.1

176.4 ± 6.7

32 150.4 22 178.0

33 157.5 23 179.8

34 142.8 24 163.3

35 175.0 25 182.4

36 162.4 26 169.8

37 166.0 27 187.9

38 149.3 28 176.4

39 161.1 29 177.3

40 157.7 30 174.3

SDW

41 180.6

171.7 ± 15.3

51 212.1

219.1 ± 7.0

42 171.7 52 231.7

43 141.9 53 225.8

44 176.1 54 217.6

45 174.4 55 215.9

46 165.0 56 213.3

47 180.1 57 221.6

48 154.3 58 221.3

49 176.4 59 215.7

50 196.5 60 216.4

SZA

71 134.3

130.1 ± 29.0

61 144.6

153.4 ± 12.3

72 109.6 62 155.4

73 130.9 63 148.5

74 118.2 64 136.5

75 109.1 65 147.2

76 133.8 66 156.4

77 164.7 67 170.4

78 112.7 68 141.2

79 95.9 69 158.8

80 191.9 70 174.9

The yield point is the weight limit that the body safely
supports before plastic deformation occurs, (i.e., an irre-
versible deformation or microstructure rearrangement that
does not allow the bone to return to its initial shape and
dimension). This variable is defined as the last point in the
linear phase (elastic phase) of the load-deformation curve.
As the yield point is a rarely studied variable, few studies
are available for comparison. ZA increased the maximum

yield point values in this study, which increased the safety
zone over which the bone microstructure remained intact
and within the limits of elastic deformation. Choosing an
ROI with a high concentration of trabecular bone may have
positively influenced these results [13–15].

The stiffness coefficient is one of the major biomechani-
cal evaluation parameters; it indicates the stability or rigidity
of the material under the maximum load. The stiffness



Journal of Osteoporosis 7

Table 4: Overview of the biomechanical parameters over time.

Group Biomechanical parameter 9 months (mean ± SD) P 12 months (mean ± SD)

ODW

ML (N) 124.2 ± 12.1 †P = 0.002 112.6 ± 8.9

YP (N) 113.0 ± 11.4 NS 105.7 ± 9.0

SC (N/mm) 214.2 ± 19.0
†P = 0.002

236.2 ± 24.4§P < 0.001

OZA
ML (N) 141.4 ± 9.8 †P = 0.003 138.7 ± 9.1

YP (N) 129.7 ± 6.0 †P = 0.02 119.8 ± 9.7

SC (N/mm) 158.2 ± 9.1 †P < 0.001 176.4 ± 6.7

SDW
ML (N) 140.0 ± 6.6 †§P < 0.001 118.4 ± 10.5

YP (N) 125.3 ± 9.1 †P = 0.01 112.6 ± 6.2

SC (N/mm) 171.7 ± 15.3 †P < 0.001 219.1 ± 7.0

SZA

ML (N) 149.7 ± 4.3 NS 151.0 ± 9.7

YP (N) 137.0 ± 10.7 NS 124.6 ± 16.8

SC (N/mm) 130.1 ± 29.0
§P < 0.001

153.4 ± 12.3†P = 0.01
†Longitudinal study design (paired t-test).
§Cross-sectional study design (ANOVA; Holm-Sidak’s post hoc).
NS: no significance.

coefficient is obtained from the relationship between the
applied load and body deformation. A higher stiffness should
be interpreted as a greater propensity to break under a fixed
deformation, which is typical of brittle materials, such as
glass. The stiffness coefficient is calculated from the linear
portion of the elastic phase of the load-deformation curve
(Figure 4). Zoledronic acid reduced the stiffness coefficient
in all groups. In other words, ZA reduced femoral stiffness
and rendered the bone to be more ductile and less likely
to fracture. In a similar study of human tibiae at different
patients ages, Burstein et al. [24] concluded that the resis-
tance (maximum load) was similar in young and elderly
individuals; however, the “old” bone was more “brittle” and
characteristic of “fragile” materials; thus, it had a greater
stiffness. Hormonal deficiency tends to increase the stiffness
coefficient, making the bone more fragile or brittle. Similar
to previous results [8, 25, 26], ZA could maintain and even
reduce the bone stiffness coefficients of the oophorectomized
animals in the present study (group OZA) to levels similar
to those of the non-oophorectomized animals (group SZA).
These results suggest that the drug maintained the absolute
(i.e., organic and inorganic) bone integrity, which would
explain the decrease in the femoral stiffness coefficient.

6. Conclusions

Zoledronic acid administered intraperitoneally at a single
dose of 0.1 mg/kg significantly increased the maximum load
and yield point and reduced the stiffness coefficient in the
proximal region of the femur of oophorectomized rats after
nine and 12 months of observation.

Conflict of Interests

The authors have no conflict of interests to declare.

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