Diabetic Foot Clinical Trial
Official title:
Efficacy and Safety of Heberprot-P® in Patients With Advanced Diabetic Foot Ulcer in Dasman Diabetes Institute. Demonstrative Study
The purpose of this study is to assess the efficacy and safety of the intralesional administration of Heberprot-P® (human recombinant epidermal growth factor) plus the standard treatment in patients with complex diabetic foot and risk of major amputation in Kuwait.
Diabetic foot ulcers constitute an important medical problem in the patients with diabetes
mellitus. The epidermal growth factor (EGF) stimulates the proliferation of fibroblasts,
keratinocytes and vessel endothelial cells, which contributes to its healing properties.In
previous phase I-III clinical studies in patients with diabetic foot ulcers grade 3 and 4 of
the Wagner's classification (Meggitt-Wagner classification), it has been demonstrated that
the intralesional administration of the EGF stimulates the healing, having as result the
formation of a useful granulation tissue in the bed of the ulcers and the later closure of
the lesion. This effect was associated with a decreased risk of amputation. Considering the
pharmacological actions identified for the EGF, the pathogenesis of the disease, previous
clinical results and the absence of an effective treatment for this condition justifies the
current clinical study. The purpose of this study is to assess the efficacy and safety of the
intralesional administration of Heberprot-P® (human recombinant epidermal growth factor) plus
the standard treatment in patients with complex diabetic foot and risk of major amputation in
Kuwait.
A demonstrative study, open, single-center, uncontrolled, with one treatment group to be
conducted in a maximum of 50 patients with DFU. The study will be conducted at DDI, Kuwait.
General objective To assess the efficacy and safety of the intralesional administration of
Heberprot-P® plus the standard treatment in patients with diabetic foot ulcer in University
of Texas Wound Classification AI-AII and CI-CII and risk of major amputation.
Specific objectives To determine the efficacy of Heberprot-P® in patients with diabetic foot
ulcer in terms of the proportion of patients that reach complete response (100% of the area
covered by granulation tissue) at the end of treatment.
To determine the time to reach the granulation tissue 100% of the lesion area. To assess the
effect of the administration of Heberprot-P® in the prevention of major amputations.
To identify and characterize the adverse events associated with the intralesional and
perilesional administration of Heberprot-P® in patients with diabetic foot.
Methods to evaluate the quality of the assessment procedures of the efficacy. Quality control
visits will be carried out during the demonstration by the Research affairs office in DDI,
Kuwait and CIGB, previously coordinated with the investigators. When the patient finishes the
treatment, the monitors will gather the CRFs leaving a copy in the research site.
Behavior in case of exit from the demonstration Management of withdrawals and missings to
evaluation visits is explained in item. The assessment will be carried out according to the
principle of intent to treat, so all the patients once included will be considered in the
response assessment, regardless they have had received the treatment or not, or having
completed the follow-up.
Adverse events to that can appear and their recording An adverse event is any medical
undesirable and not deliberate manifestation that happens in a patient or subject of a
clinical research to which a drug has been administered, regardless if it is related or not
to this treatment.
This way, it can be any sign (including for example abnormal laboratory data), symptoms or
disease associated temporarily with the use of a pharmaceutical product, being or not a
causality ratio. The exacerbations of symptoms/diseases that were present before the study
will also be included as adverse events.
In the post-marketing stage, during the active pharmaco-surveillance of the use of
Heberprot-P® there were included about 4000 subjects. In the initial analysis of 1851
patients, 873 patients reported adverse events, the most frequent were: pain at the site of
application (21.7%), shivering from cold (19.8), burning at the application site (16.0%),
chills (9.2%), local infection (3.8%) and fever (2.3%).
All the information related to the occurrence of adverse events presented in the patients
included in the clinical demonstration will be registered and described by the researchers in
the Adverse Events Form of the CRF. There will be described the type, duration, intensity,
seriousness, causality and the followed behavior.
The intensity (severity) will be classified the following way:
1. Mild: adverse event that the subject tolerates well, causes minimal inconveniences and
does not interfere with the daily activities.It does not need treatment and does not
interrupt the administration.
2. Moderate: adverse event that is annoying enough as to interfere the daily activities. It
needs treatment and not necessarily needs the suspension of the causative drug.
3. Severe: adverse event that prevents from doing the daily activities.
The criteria that will be used to define an adverse event as serious will include the
presence of some of the following conditions:
It endangers the subject's life causes the death causes or prolongs the hospitalization
produces disability/incapacity causes congenital anomaly
These events need the suspension of the causative drug.
Behavior in case of adverse events The most frequent clinical adverse events reported with
the use of Heberprot-P are pain and Burning sensation in the injection site, shivering,
chills, local infection and fever. The behavior in case of these adverse events includes the
administration of antibiotics.
In case allergic reactions appear, the behavior will depend on their magnitude, including the
use of antihistamines, steroids or even definitive suspension of the treatment.
In case of having serious adverse events, the treatment will be suspended, there will be
taken the measures needed depending on the type of event and it will be considered the
possible expeditious report of the event.
Expeditious report of the adverse events Any unexpected serious adverse event that appears in
the course of the clinical demonstration will be valued with a view to the expeditious
report. The term "unexpected" refers to the events which specificity or seriousness is not
consistent with the available information of the product (Annex 3).
In case you have a serious and unexpected adverse effect, the Clinical investigator will
report to Dr Rafael Ibargollin Ulloa and DDI Ethics committee .
Follow up as for all reportable AEs. Basic follow up information must also be documented on
the SAE Report Form and in the CRF.
Recording of the information and handling the data
- Researcher´s registry. After the patient has been included Patient´s identification
data.
- Registry of Included and Not included Patients. During the whole period of inclusion of
cases List of all the patients with diagnosis who come to the participant service,
indicating if they were included or not and the causes of non-inclusion.
- Informed consent Before the inclusion Record of the patient's voluntariness in taking
part in the study.
- Case Report Form. At the beginning and during the patient's follow-up. General data,
clinical assessments and complementary examinations.
- Serious adverse event notification form. When serious and unexpected adverse events are
faced. Patient's data, description of the adverse events, date and time of start and
completion, behavior, causality ratio and result.
The information specified in the CRF will be completed by researchers in each of the
assessments. When patients have completed follow-up, the CRF should be reviewed and signed.
The CRF will be filled in duplicate, the researcher will keep a copy and send the other to
the monitors in the CIGB. Informed consent will also fill in duplicate, one for the
investigator and the other to the patient.
With the individual data a database will be created, which will serve for their processing. A
double entry of the data will be carried out for later comparison and correction from
possible errors.
Procedure for preserving the information The CRFs, the databases, the reports that are
generated and the compact discs with the images will be preserved in the site destined for
this effect, previously designated by the persons in charge of the demonstration and they
will be preserved for at least 15 years by the sponsor.
Exploratory analysis of the data The analyses will be carried out by intention to treat,
considering the abandonments as non-responses to the treatment.
With each variable (main, secondary and control) exploratory analyses will be carried out to
know their global behavior and to evaluate fulfillment of the necessary hypothesis in order
to apply the proper statistical tests in the assessment stage.With the quantitative
variables, the assumptions of homogeneity of variances (Levene's test) and of approximation
to a normal distribution (Shapiro-Wilk's test) must be verified. Additionally, as
measurements of central tendency and dispersion, the mean, median, standard deviation,
interquartile range and minimum and maximum values will be estimated. With the qualitative
variables, the distribution of frequencies should be estimated. It is proposed to carry out a
Cluster Analysis as exploratory method of association between the variables.
Homogeneity of the sample With the qualitative variables (sex, type of Diabetes Mellitus,
obesity, smoking arterial hypertension, structural deformities, consumption of alcohol,
current treatment for the diabetes, history of ulcers, location of the lesion, osteomyelitis,
DDI, University of Texas Wound Classification System.
The frequency distribution will be estimated. With the quantitative variables (age, time of
evolution of the diabetes mellitus and of the ulcer, glycosylated hemoglobin, initial area of
the lesion, ankle/arm pressure index at the beginning): The measurements of central tendency
and dispersion will be estimated and analysis of normality will by made (Shapiro-Wilk's
tries) and of homogeneity of variances (Levene's test).
With all (quantitative and qualitative variables): A logistic regression model will be
adjusted to study the influence of each of them and their interactions on the response to the
treatment and occurrence of serious adverse events. In case any statistically significant
dependence(s) is/are detected, the confirmatory analysis with the main variable should
envisage it/them as covariable (s) or stratum (strata).
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