Objective: The present work aims to analyse the effectiveness of platelet-rich plasma (PRP) in degenerative knee pathology based on real-world data and to evaluate possible factors influencing the response to treatment. Methods: In total, 531 cases were analysed collecting data on gender, age, body mass index, pathology location, severity, number of cycles and route of administration. Clinical outcome was evaluated at 6 and 15 months after treatment, using the Knee injury and Osteoarthritis Outcome Score (KOOS) and obtaining percentages of Minimal Clinically Important Improvement (MCII). Blood and PRP samples were randomly tested as a quality control measure to ensure the correct properties. Comparative statistical tests and multivariate regression were performed for the analysis of the variables. Results: The PRP applied had a platelet concentration factor of 1.67, with no leukocytes or erythrocytes. The percentage of patients with MCII at 6 and 15 months after PRP application was 59.32% and 70.62%, respectively. Patients with MCII were younger (p = 0.0246) and with lower body mass index (p = 0.0450). The treatment had a better response in mild/moderate cases than in severe cases (p = 0.0002). Intraosseous PRP application in severe cases improved the effect of intraarticular PRP (p = 0.0358). The application of a second cycle of PRP only improved the response in patients without MCII at 6 months (p = 0.0029), especially in mild/moderate cases (p = 0.0357). Conclusion: The applications of PRP in degenerative knee pathologies is an effective treatment, but this effectiveness nonetheless depends on several variables. Real-world data can complement that from clinical trials to provide valuable information.
Objective: The present work aims to analyse the effectiveness of platelet-rich plasma (PRP) in degenerative knee pathology based on real-world data and to evaluate possible factors influencing the response to treatment. Methods: In total, 531 cases were analysed collecting data on gender, age, body mass index, pathology location, severity, number of cycles and route of administration. Clinical outcome was evaluated at 6 and 15 months after treatment, using the Knee injury and Osteoarthritis Outcome Score (KOOS) and obtaining percentages of Minimal Clinically Important Improvement (MCII). Blood and PRP samples were randomly tested as a quality control measure to ensure the correct properties. Comparative statistical tests and multivariate regression were performed for the analysis of the variables. Results: The PRP applied had a platelet concentration factor of 1.67, with no leukocytes or erythrocytes. The percentage of patients with MCII at 6 and 15 months after PRP application was 59.32% and 70.62%, respectively. Patients with MCII were younger (p = 0.0246) and with lower body mass index (p = 0.0450). The treatment had a better response in mild/moderate cases than in severe cases (p = 0.0002). Intraosseous PRP application in severe cases improved the effect of intraarticular PRP (p = 0.0358). The application of a second cycle of PRP only improved the response in patients without MCII at 6 months (p = 0.0029), especially in mild/moderate cases (p = 0.0357). Conclusion: The applications of PRP in degenerative knee pathologies is an effective treatment, but this effectiveness nonetheless depends on several variables. Real-world data can complement that from clinical trials to provide valuable information.
Knee joint degeneration is a highly disabling disease, especially in the elderly
population, with a prevalence of more than 15% worldwide, and more than 40% in
patients over 40 years of age.
Today’s habits such as sedentarism, obesity and an ageing population will
inevitably lead to an increase in prevalence in the coming years, not only in the
elderly population but also in young patients.
Its complexity is another obstacle that makes it a challenge for health
systems, because other structures besides the cartilage are involved, namely, the
synovial membrane and the subchondral bone.
The lack of a clear therapeutic target and its degenerative nature make it
difficult to apply effective treatment to stop or slow its progression. Current
treatments, such as oral or intraarticular pharmacology, achieve symptom relief but
do not resolve this disease, making total knee arthroplasty the definitive solution
for these patients. However, this surgical intervention is contraindicated in
patients of advanced age or with multiple comorbidities, not to mention the inherent
surgical risks and associated costs.[4,5]Treatments based on regenerative medicine, such as platelet-rich plasma (PRP) or cell
therapies, aim to expand therapeutic arsenal so as to avoid or delay surgery as far
as possible. While cell therapy is still in its infancy and has to overcome several
challenges, PRP has been applied for more than 15 years with a consolidated position
in the treatment of this disease.
It is based on obtaining the plasma fraction from the patient’s blood with a
concentration of platelets similar to or higher than in blood levels. PRP contains
high levels of biomolecules that participate in different biological processes that
favouring cellular repair.An increasing number of randomized clinical trials (RCTs) are being conducted to draw
firm conclusions regarding the efficacy and safety of PRP, with promising results.
Although RCTs are the cornerstone of evidence-based medicine, their use for
the study of PRP has certain limitations. The term PRP encompasses a range of
products of different compositions, which makes a proper comparison between the
different studies impossible and leads to contradictory results. This also prevents
the aggregation of patients from different RCTs for the analysis of large population
samples. On the contrary, the information obtained from real-world evidence (RWE)
studies may be a useful complement to the data obtained from RCTs. RWE can be
defined as the collection of clinical data from patients in routine clinical
practice. Although it does not have all the strengths of RCTs, it allows the
real-world data collection from a large volume of patients and the assessment of
various factors that may influence treatment.[9,10] The combination of both types
of study provides the medical and scientific community with valuable information for
the further study of pathologies and treatments. However, there are hardly any RWE
studies on knee degeneration and PRP.[11,12]We hypothesize that conducting RWE studies could provide information to help optimize
treatment protocols. Thus, the present work aims to analyse the effectiveness of PRP
in knee degenerative pathology, based on a large number of patients, and to evaluate
possible factors influencing the response to treatment.
Methods
Study design, patients and data collection
The study was designed as a prospective observational study to analyse PRP
application in knee degenerative pathology. This study was carried out in
accordance with the International Declaration of Helsinki in Fortaleza, Brazil
(2013), Good Clinical Practice Regulations and the STROBE (Strengthening the
Reporting of Observational Studies in Epidemiology) statement.
Ethical approval for this study (Protocol No. EPA2015046) was obtained
from the Ethics Committee of the Basque Country (September 2015), as was written
informed consent.The eligible patients were enrolled consecutively between 2015 and 2020 in the
same medical centre. They met the following inclusion criteria: patients of both
sexes over 18 years old, diagnosed with knee joint degeneration and a complete
follow-up for a minimum of 12 months. The exclusion criteria were as follows:
associated joint pathologies or systemic autoimmune rheumatic disease, and any
knee intervention or intraarticular infiltrations in the past 12 months or
during PRP treatment and follow-up.Age, sex, body mass index (BMI), number of PRP cycles (one or two), route of
administration (intraarticular or intraosseous), presence of synovial fluid,
location and pathological severity were collected. Imaging studies assessed
pathological severity using the Ahlbäck and Outbridge scales for osteoarthritis
and chondropathies, respectively. Patients were divided into two categories:
mild or moderate grade (Ahlbäck: I–II; Outbridge: 1–2) and severe grade
(Ahlbäck: III–IV, Outbridge 3–4). Patients completed the Knee injury and
Osteoarthritis Outcome Score (KOOS) to assess their response to treatment.
Concurrent medication such as paracetamol was forbidden 48 h before assessment.
All data were collected through the use of electronic medical records.
PRP preparation
Depending on whether infiltration was intraarticular or intraosseous, 32 or 80 ml
of venous blood was extracted from the patient, respectively. The blood was
withdrawn into 9-ml tubes containing 3.8% (w/v) sodium citrate and centrifuged
at 580 × g for 8 min at room temperature (BTI Biotechnology
Institute, Vitoria-Gasteiz, Spain). The 2-ml plasma fraction located above the
red blood fraction, but not including the buffy coat, was collected. This plasma
fraction contained a moderate concentration of platelets (1.5–2.5 times compared
with peripheral blood) and an absence of erythrocytes and leukocytes. Calcium
chloride (10% w/v) was added as an activator. All procedures were performed
under sterile conditions.
PRP quality control
During routine clinical practice, blood and PRP samples are collected randomly
and periodically from patients undergoing treatment. Both types of samples are
analysed in the Sysmex XS-1000i haematology analyser (Sysmex, Kobe, Japan) to
verify that the PRP is elaborated correctly and complies with the parameters
indicated by the manufacturer.
Treatments
The intraarticular administration consisted of 8 ml of PRP infiltrated into the
articular space after evacuating the totality of the synovial fluid. One PRP
cycle consisted of three intraarticular infiltrations on a weekly basis.In the first treatment visit, intraosseous administration included three
different injections of 2 ml (patella) and 5 ml (femoral head and tibial
plateau) into different anatomical locations, conducted in the operating room.
Following one PRP intraarticular injection, two PRP intraosseous injections were
performed depending on the location of the degeneration, in accordance with the
technique described by Sánchez et al.
Two more intraarticular PRP infiltrations were performed over the 2 weeks
following the first visit to complete the PRP administration cycle.In both cases, patients could opt for a second PRP cycle approximately 6 months
after the first, depending on the physician’s recommendation after a follow-up
visit which consisted of a clinical and physical evaluation.
Outcome evaluation
Patients filled out KOOS at baseline, 6 months and 15 months (a follow-up window
of between 12 and 18 months) after the third injection of the first cycle of
PRP. The primary efficacy criterion was a change from baseline in joint pain,
measured using the KOOS pain subscale. Success rates were calculated according
to a reduction in the pain score of at least 10 points from baseline (Minimal
Clinically Important Improvement (MCII)).
Secondary variables included changes in KOOS subscales for symptoms,
activities of daily living (ADL), function in sport and recreation (Sport/Rec)
and knee-related quality of life (QOL).
Statistical analyses
Demographic and medical variables were determined by the mean and standard
deviation for parametric data, and median and 95% confidence interval (CI) for
non-parametric data. A comparison of the patients’ success rate percentages was
carried out using the χ2 test. Comparisons were performed by
Student’s t test for independent or paired parametric data,
Wilcoxon signed-rank test for paired non-parametric data and Mann–Whitney
U test for independent non-parametric data. Multivariate
logistic regression was performed to analyse the influence of the different
variables considered collectively, calculating coefficients
(B), p value, odds ratios (ORs) and 95% CI.
Distribution of the samples was assessed by Shapiro–Wilk’s test. Data were
considered statistically significant when p < 0.05.
Statistical analysis was performed with SPSS 20.0 (SPSS, Chicago, IL, USA).
Results
PRP characterization
A total of 445 blood samples and corresponding PRP sample were analysed at
random. The median PRP platelet concentration was
309 × 103 platelets/ml (CI: 297–327), reaching a concentration factor
of 1.67 (CI: 1.63–1.73), and with no leukocytes or erythrocytes. In accordance
with the latest coding system and minimum reporting requirements for PRP
studies, the PRP used in this study was 13-00-11, and the characteristics of the
PRP are reported in Table
1.
Table 1.
Characteristics of platelet rich-plasma.
Parameter
Values
PRP preparation
Initial blood volume
32 ml (intraarticular) or 80 ml (intraosseous)
Anticoagulant
Sodium citrate 3.8% (w/v)
System
Close
Centrifugation
Yes
Number
1
Speed
580 × g for 8 min
Final PRP volume
8 ml (intraarticular) or 20 ml (intraosseous)
PRP characteristics
PRP type
13-00-11
MPV
9.60 fl (CI: 9.50–9.80)
Red blood cells
<0.01 × 106/µl
White blood cells
<0.05 × 106/µl
Neutrophils
–
Lymphocytes
–
Monocytes
–
Eosinophils
–
Basophils
–
Activation
CaCl2 (10% w/v)
Application characteristics
Formulation type
Liquid
Administration route
Intraarticular or intraosseous
Dosage
3 infiltrations on a weekly basis
Volume
Intraarticular injection: 8 mlIntraosseous
injection: 3–5 ml
CI, confidence interval; PRP, platelet-rich plasma; MPV, mean
platelet volume.
Characteristics of platelet rich-plasma.CI, confidence interval; PRP, platelet-rich plasma; MPV, mean
platelet volume.
Demographics, the overall effectiveness of PRP and influence of patient
factors
The study analysed a total of 441 patients (531 knees; Figure 1). The median age was
60.47 years (CI: 59.41–61.87), with a mean BMI of 28.65 (CI: 28.09–29.25) and a
percentage of females of 47.47%. The percentage of cases who showed a pain
reduction of at least 10 points (MCII) from baseline to 6 months was 59.32% (315
out of 531), and 70.62% (375 out of 531) by 15 months. All KOOS scores showed a
significant statistical increase at 6 months post-treatment, with improvement
maintained at 15 months post-treatment (p < 0.0001; Figure 2).
Figure 1.
Study flowchart. Selection of eligible patients and distribution of cases
analysed according to severity and treatment.
BML, bone marrow lesion; PRP, platelet-rich plasma.
Figure 2.
Overall effectiveness of platelet-rich plasma. Percentage of MCII
patients at 6 and 15 months after treatment (a). KOOS scores before and
after treatment (b).
ADL, activities of daily living; CI: confidence interval; KOOS, Knee
injury and Osteoarthritis Outcome Score; MCII, Minimal Clinically
Important Improvement; QOL, knee-related quality of life; Sport/Rec,
function in sport and recreation.
Study flowchart. Selection of eligible patients and distribution of cases
analysed according to severity and treatment.BML, bone marrow lesion; PRP, platelet-rich plasma.Overall effectiveness of platelet-rich plasma. Percentage of MCII
patients at 6 and 15 months after treatment (a). KOOS scores before and
after treatment (b).ADL, activities of daily living; CI: confidence interval; KOOS, Knee
injury and Osteoarthritis Outcome Score; MCII, Minimal Clinically
Important Improvement; QOL, knee-related quality of life; Sport/Rec,
function in sport and recreation.Error bars: CI. *p < 0.05;
**p < 0.001; ***p < 0.0001.Patients with MCII at both 6 and 15 months were significantly younger than those
not experiencing clinical improvement, with a median age of 62 years at 6 months
(CI: 60–64) compared with 65 years (CI: 63–66) (p = 0.0137). At
15 months, the age of patients with MCII (62; CI: 60–63) was significantly lower
than that of patients without MCII (65; CI: 64–67)
(p = 0.0246). Concerning BMI, at 15 months, patients with MCII
(27.62; CI: 27.00–28.23) presented a BMI significantly lower than that of
patients without MCII (28.03; CI: 27.41–29.51)
(p = 0.0450).
Influence of pathology factors: severity and location
Of the 531 cases, 39.36% (209 out of 531) were mild/moderate, and the response of
these was 66.03% at 6 months and 79.90% at 15 months, 11.06 percentage points
higher than the severe cases at 6 months (CI: 2.52–19.23;
p = 0.0113) and 15.31 percentage points higher at 15 months
(CI: 7.52–22.56; p = 0.0002) (Figure 3). The difference in scores for
increase in pain (p = 0.0040) and Sport/Rec
(p = 0.0457) between these two groups was also significant.
There was no difference in age (p = 0.3611) or BMI
(p = 0.24.96) between patients in the two severity
groups.
Figure 3.
Percentage of patients with MCII according to severity and route of
administration.
6M, follow-up at 6 months; 15M, follow-up at 15 months; MCII, Minimal
Clinically Important Improvement.
*p < 0.05; **p < 0.001 with
respect to severe cases; #p < 0.05 with
respect to severe cases treated with intraarticular infiltrations.
Percentage of patients with MCII according to severity and route of
administration.6M, follow-up at 6 months; 15M, follow-up at 15 months; MCII, Minimal
Clinically Important Improvement.*p < 0.05; **p < 0.001 with
respect to severe cases; #p < 0.05 with
respect to severe cases treated with intraarticular infiltrations.Of the cases, 48% presented synovial fluid leakage in the knee (254 out of 531),
this being a significant feature in severe osteoarthritis with a difference of
22.05 (CI: 14.41–30.16) percentage points compared with mild/moderate
pathologies (p < 0.0001). The presence of synovial fluid did
not influence treatment efficacy. At 6 and 15 months post-treatment, the
percentage of patients with no more joint effusion was 73.62% and 68.50%,
respectively.The extension of degeneration did not influence the clinical outcomes of PRP
(Supplementary Table S1). In unicompartmental pathologies,
mild/moderate cases affecting the patellofemoral joint achieved a better result
than tibiofemoral cases of the same grade (Supplementary Table S2). Those patients were much younger
(39 years; CI: 35–45) and had a lower BMI (25.50; CI: 24.02–25.90) than those
with mild/moderate tibiofemoral degeneration (66 years; CI: 64–48 and 28.48; CI:
26.96–30.88). Detailed analysis of all locations showed no difference in
treatment response (Supplementary Table S3).
Influence of protocol factors: PRP cycles and administration route
Of all the cases analysed, 117 opted for a second PRP cycle after the first
follow-up period, 63 without MCII at 6 months and 54 with a positive response
(Figure 4). Of the
first 63 patients, 37 achieved MCII after the second PRP cycle (58.73%),
22.13 points higher than the group showing no MCII at 6 months and that did not
receive a second cycle of PRP (CI: 7.51–35.54; p = 0.0029).
This improvement was only observed in mild/moderate pathologies, with 25.25
percentage points more in the group with the second cycle of PRP (CI:
1.93–44.82.54; p = 0.0357; Supplementary Table S4). In terms of the effect of a second PRP
cycle in sustaining the effect of treatment over time, there was no difference
between the 54 patients with MCII at 6 months who opted for a second PRP cycle
versus those who did not repeat the PRP cycle
(p = 0.1951; Supplementary Table S5).
Figure 4.
Percentage of patients with MCII according to number of cycles of
PRP.
15M, follow-up at 15 months; MCII, Minimal Clinically Important
Improvement; PRP, platelet-rich plasma.
*p < 0.05 with respect to the group receiving one PRP
cycle.
Percentage of patients with MCII according to number of cycles of
PRP.15M, follow-up at 15 months; MCII, Minimal Clinically Important
Improvement; PRP, platelet-rich plasma.*p < 0.05 with respect to the group receiving one PRP
cycle.Of the 531 cases, 307 received intraarticular treatment, with 59.61% of patients
(183 out of 307) showing MCII at 6 months and 72.31% at 15 months (222 out of
307). This improvement was greater in mild/moderate pathology cases, at 66.03%
(138 out of 209) and 79.90% (167 out of 209), respectively. However, in severe
pathologies, MCII was 45.91% (45 out of 98) at 6 months and 56.12% (55 out of
98) at 15 months (Figure
3). The increase in KOOS scores was also significantly greater in
mild/moderate cases than in severe cases (Figure 5(a) and (b)).
Figure 5.
Differences in response according to severity and route of
administration. Differences in the increase in KOOS scores according to
severity after intraarticular PRP treatment at 6 (a) and 15 (b) months
follow-up. Differences in the increase of KOOS scores according to the
type of treatment in severe pathologies at 6 (c) and 15 (d) months
follow-up.
ADL, activities of daily living; KOOS, Knee injury and Osteoarthritis
Outcome Score; QOL, knee-related quality of life; Sport/Rec, function in
sport and recreation.
Differences in response according to severity and route of
administration. Differences in the increase in KOOS scores according to
severity after intraarticular PRP treatment at 6 (a) and 15 (b) months
follow-up. Differences in the increase of KOOS scores according to the
type of treatment in severe pathologies at 6 (c) and 15 (d) months
follow-up.ADL, activities of daily living; KOOS, Knee injury and Osteoarthritis
Outcome Score; QOL, knee-related quality of life; Sport/Rec, function in
sport and recreation.Error bars: CI. *p < 0.05;
**p < 0.001; ***p < 0.0001.The effectiveness in treating severe pathologies was significantly improved when
PRP was administered via intraosseous route. Of the 531 cases,
224 received intraosseous treatment, all with severe pathology. When comparing
the clinical outcome in severe pathology, the group receiving intraosseous PRP
had an MCII rate of 58.92% at 6 months, 13.01 percentage points higher compared
with patients receiving intraarticular treatment (CI: 1.19–24.39;
p = 0.0311). The MCII rate at 15 months was 68.30%,
12.18 percentage points higher than the response to intraarticular PRP (CI:
0.82–23.59; p = 0.0358; Figure 3) (Supplementary Table S6). Increases in KOOS scores were also
greater in cases treated with intraosseous PRP (Figure 5(c) and (d); Supplementary Table S7).
Bone marrow lesions
In 33 of the 531 cases, bone marrow lesions (BMLs) were detected by magnetic
resonance imaging (MRI) and treated with intraosseous PRP. The average age of
this group of patients was 49 ± 14.82 years with a BMI of 26.96 ± 4.25 and a
female percentage of 42.42%.The percentage of patients with MCII at 6 and 15 months post-treatment was 69.70%
(23 out of 33) and 78.79% (26 out of 33), respectively. All KOOS scores improved
significantly at both 6 and 15 months post-treatment
(p < 0.001). During follow-up MRI studies, the decrease
(41.94%) and removal (41.94%) of the BML image were observed (Figure 6).
Figure 6.
MRI images of BML. Before (a) and 15 months after (b) intraosseous PRP
treatment of a BML in the medial femoral condyle. Before (c) and
15 months after (d) intraosseous PRP treatment of a BML in the tibial
plateau.
BML, bone marrow lesion; MRI, magnetic resonance imaging.
MRI images of BML. Before (a) and 15 months after (b) intraosseous PRP
treatment of a BML in the medial femoral condyle. Before (c) and
15 months after (d) intraosseous PRP treatment of a BML in the tibial
plateau.BML, bone marrow lesion; MRI, magnetic resonance imaging.
Multivariate logistic regression
The multivariate logistic regression model indicated that medium/moderate
severity (p = 0.001) and intraosseous application
(p = 0.024) significantly favoured positive response to
treatment at 6 months (Table 2). The 12-month model (Table 3) showed the strong influence
of severity, with a better response in patients with mild/moderate pathologies
(p < 0.001).
Table 2.
Multivariate regression analysis for response at 6 months.
Variable
B
p value
95% CI
OR
Age
–0.008
0.291
0.977–1.007
0.992
BMI
–0.017
0.408
0.943–1.024
0.983
Severity (mild–moderate/severe)
0.870
0.001*
1.397–4.076
2.387
Administration route (IA/IO)
–0.604
0.024*
0.324–0.923
0.546
B, coefficient; BMI, body mass index; CI, confidence
interval; IA, intraarticular; IO, intraosseous; OR, odds ratio.
p < 0.05.
Table 3.
Multivariate regression analysis for response at 15 months.
Variable
B
p value
95% CI
OR
Age
−0.008
0.378
0.975−1.009
0.992
BMI
−0.039
0.086
0.921–1.005
0.962
Severity (mild–moderate/severe)
1.145
<0.001*
1.757–5.615
3.141
Administration route (IA/IO)
−0.473
0.088
0.362–1.073
0.623
PRP cycles
0.123
0.657
0.658–1.942
1.130
B, coefficient; BMI, body mass index; CI, confidence
interval; IA, intraarticular; IO, intraosseous; OR, odds ratio; PRP,
platelet-rich plasma.
p < 0.05.
Multivariate regression analysis for response at 6 months.B, coefficient; BMI, body mass index; CI, confidence
interval; IA, intraarticular; IO, intraosseous; OR, odds ratio.p < 0.05.Multivariate regression analysis for response at 15 months.B, coefficient; BMI, body mass index; CI, confidence
interval; IA, intraarticular; IO, intraosseous; OR, odds ratio; PRP,
platelet-rich plasma.p < 0.05.
Discussion
The present study examines 531 cases of degenerative knee pathology treated with PRP
and followed up for at least 1 year. The overall effectiveness of PRP was more than
70%, based on the percentage of patients with MCII. This response is influenced by
patient, pathology, product and protocol (4P) factors. Thus, these ‘four Ps’ should
be taken into consideration in order to achieve an optimal clinical outcome (Figure 7).
Figure 7.
The ‘four Ps’ influencing the effectiveness of PRP. The clinical response to
PRP treatment is influenced by many factors related to the patient, the
pathology, the product and the protocol, many of which are still
unknown.
PRP, platelet-rich plasma.
The ‘four Ps’ influencing the effectiveness of PRP. The clinical response to
PRP treatment is influenced by many factors related to the patient, the
pathology, the product and the protocol, many of which are still
unknown.PRP, platelet-rich plasma.RWE studies are a valuable tool to analyse the effectiveness of treatment in a real
scenario and the factors that may influence it. Although RCTs are essential to
evidence-based medicine, they present several limitations that hinder this type of
analysis. Concerning PRP, RCTs evaluate a limited number of subjects, and although
they are subsequently examined in meta-analyses, the data obtained can be misleading
due to the different PRP products and treatment protocols. In contrast, despite
their inherent limitations, RWE studies reflect the response to treatment in the
real world and allow us to reach a sufficient number of patients to analyse the
different variables that could influence the response. The information obtained in
both types of studies is useful in helping to find the best possible
treatment.[9-11]The present study is the prospective observational study to have analysed the largest
number of patients to date. The results obtained align with the latest RCTs and
meta-analyses published, indicating that PRP is an effective treatment for
degenerative knee pathologies. Our work considers clinical outcome the results of
the scores and their clinical significance according to the MCII, because a
statistically significant difference in the scores does not mean a clinical
one.[8,10-21] This is becoming increasingly
important in the analysis
and allows a better interpretation.
It should be noted that the type of PRP applied to all the patients in the
study was obtained using the same system and with the same cellular composition in
accordance with the quality control carried out, so it is a variable that did not
interfere in the results analysed.The only study with similar characteristics that can be compared with the present
work was that carried out by Korpershoek et al.,
which analysed 158 cases treated with Autologous Conditioned Plasma (ACP).
The authors obtained similar results to ours in terms of KOOS scores, with
significant differences at 6 and 12 months from baseline. However, the MCII values
are lower, which may be due to several factors such as patient characteristics.
While the work of Korpershoek et al. focuses only on knee
osteoarthritis, the present work encompasses all joint degeneration. We must
underline the high efficacy (more than 90%) of the treatment in cases of
chondromalacia patellae, which correspond to mild/moderate cases of patellofemoral
pathology. Although the data obtained do not suggest the influence of location on
the efficacy of the treatment, the typology of these patients,
with early degeneration, young age and low BMI, makes them highly suitable
candidates for PRP treatment, as these are key factors in the response to treatment
according to the data obtained. In the case of age, the enhanced response could be
due to improved health and the molecular composition of the PRP.
Very few studies have evaluated the effect of PRP in chondromalacia patellae
achieving good results both in imaging and clinical studies.[27-29] This treatment should be
considered an option not only for the improvement of the patient but also to attempt
to prevent more serious conditions such as patellofemoral osteoarthritis.A second key factor is the type of product and the application protocol. Korpershoek
et al. used ACP that is similar to that used in our study. This
PRP does not present leukocytes and erythrocytes, which could make it the most
suitable for this type of pathology.[30,31] However, the platelet
concentration reached by Korpersoek et al. doubled ours and was
applied in a volume of only 3–5 ml, compared with 8 ml in our protocol. It makes the
number of platelets similar in each intraarticular infiltration (around
2.5×109 ) in a different volume. Furthermore, a recent RCT that
failed to demonstrate the superiority of PRP versus placebo used a
type of PRP with a large variability in concentration factor (1.6×–5×) and a volume
of 5 ml.
Thus, not only the type of product but also the volume needs to be kept in
mind. The intraarticular distribution of the PRP must be adequate and reach all the
tissue, which is achieved with volumes of approximately 9 ml.
Guillibert et al.
observed that a high-volume (8 ml) administration of PRP achieved a clinical
improvement of more than 80%, proposing this administration as a better alternative
to repeated low-volume infiltration protocols. Furthermore, injecting smaller
volumes would also lead to the delivery of less therapeutic content present in the
plasma such as exosomes or other biomolecules.[35,36]Regarding the treatment protocol, previous clinical studies suggest that repeated
weekly PRP injections are more effective than a single dose.
In addition, kinetic studies showed a release of biomolecules from fibrin
during 1 week.
However, the application of repeated PRP cycles over time is still little
studied. According to the present work, the effect of a second cycle after the first
6 months could be a useful recommendation in certain cases. In an RCT conducted by
Vaquerizo et al.,
using the same PRP and the same protocol, the authors observed an improvement
in symptoms and functionality in patients with two cycles, but not in pain, as in
the present study. However, this occurred in cases that had not yet shown a positive
clinical response at 6 months. In severe cases, it did not increase efficacy, being
effective only in patients with mild/moderate pathology. Therefore, although the
application of the second cycle of PRP would be advisable to enhance or accelerate
the response in patients with mild/moderate pathology, severe pathologies present
characteristics and a degree of complexity for which intraarticular application may
be insufficient.
Patients with severe pathologies treated with intraosseous PRP showed a
significant improvement compared with those who received only intraarticular PRP. In
these cases, key tissues such as the subchondral bone are more greatly affected. The
data obtained in the multivariate analysis confirmed the importance of the severity
of the pathology, as well as the higher impact of the route of administration
compared with the repetition of cycles. Direct application of PRP extends the range
of action and acts on detrimental processes such as the growth of fibroneurovascular
tissue, mesenchymal stem cell alterations or biomolecular imbalance.
Recent clinical studies suggest the effectiveness and safety of this
technique and are consistent with the data obtained in this study, although further
study of this route of administration is needed.
In fact, this administration could be used for other products such as cell
concentrates, although in these cases numerous variables such as age, dosage,
composition, protocol or adjuvant substances must be taken into consideration
because, otherwise, optimal clinical results may not be achieved.
Intraosseous PRP in patients with BML was also shown to be highly effective
in line with a recent study that showed a significant decrease in pain 1 year after treatment.
These subchondral bone lesions are associated with cartilage loss, and they
can also be the origin of joint degeneration.The effective results obtained in this work together with the limited adverse
effects, characterized by episodes of pain in the infiltration area during the
following hours, suggest that the reasonable application of PRP is a valid treatment
in the management of these pathologies. Along with RCT and RWE studies,
cost-effectiveness should also be taken into account for a full assessment of this
treatment. Recent studies indicate that PRP could be cost-effective in the long
term, although further research is needed.[44,45]The limitations of this study are inherent to RWE studies, which lack the strengths
of RTCs, namely, randomization, control and more specific follow-up times. The loss
of patients during follow-up is considerable, hampering longer follow-ups which
could provide important information as in previous studies,
and making it necessary for large-scale recruitment. Furthermore, despite a
large number of patients, ‘N’ was insufficient to draw solid
conclusions for some subgroups. Finally, this type of study assesses clinical
outcomes which may be due to an improvement in symptomatology rather than a
modification of the disease. However, findings such as the disappearance of BML or
reduction in joint effusion after treatment could suggest an effect on the origin of
this pathology. Indeed, the presence of synovial fluid was reduced in more than 60%
of patients after treatment, which could be a sign of a positive impact on the
progression of the disease.
In this regard, a recent work conducted by Boffa et al.
reviewed in vivo studies demonstrating disease modification
by PRP administration. Evaluation of these modifications in clinical research using
imaging or surgical studies
would help to clarify the action of PRP and its mechanisms.
Conclusion
The application of PRP in degenerative knee pathologies is an effective treatment,
but this effectiveness nonetheless depends on several variables. Far from
considering PRP to be a magic bullet, the physician must consider certain variables
related to the patient, the pathology, the product and the protocol to optimize this
treatment. Complementing the information from RCTs with that obtained from RWE
studies can be a valuable tool for advancing our understanding of PRP.Click here for additional data file.Supplemental material, sj-docx-1-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal DiseaseClick here for additional data file.Supplemental material, sj-docx-2-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal DiseaseClick here for additional data file.Supplemental material, sj-docx-3-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal DiseaseClick here for additional data file.Supplemental material, sj-docx-4-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal DiseaseClick here for additional data file.Supplemental material, sj-docx-5-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal DiseaseClick here for additional data file.Supplemental material, sj-docx-6-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal DiseaseClick here for additional data file.Supplemental material, sj-docx-7-tab-10.1177_1759720X221100304 for Real-world
evidence to assess the effectiveness of platelet-rich plasma in the treatment of
knee degenerative pathology: a prospective observational study by Mikel Sánchez,
Cristina Jorquera, Leonor López de Dicastillo, Nicolás Fiz, Jorge KnKnörrrr,
Maider Beitia, Beatriz Aizpurua, Juan Azofra and Diego Delgado in Therapeutic
Advances in Musculoskeletal Disease
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