Graft-vs-Host Disease Clinical Trial
Official title:
Vulvovaginal Graft Versus Host Disease in Women Who Underwent Transplantation Before and After Menarche
The study will evaluate the prevalence and characteristics of vulvovaginal graft versus host disease (VV- GVHD) in patients who underwent hematopoietic stem cell transplantation (HSCT) as girls or adolescents and will compare the prevalence, characteristics and severity of VV-GVHD before and after menarche.
The phenomenon of vulvovaginal graft versus host disease (VV-GVHD) following hematopoietic
stem cell transplantation (HSCT) was first described in 1982 [Corson]. It is characterized by
vulvovaginal inflammation, scarring, adhesions and might end with complete vaginal
obliteration. Hematopoietic stem cells source for the allogeneic transplantation was found to
affect the incidence of VV-GVHD: peripheral blood progenitor cells were associated with an
incidence of 50% [Zantomio], while bone-marrow harvested cells were associated with an
incidence of 25% [Spinelli].
Due to the high incidence of genital GVHD and its severe consequences we established a clinic
designated for post- transplantation patients at the Hadassah University Hospital in
Jerusalem. In a two years follow-up we found an incidence of 54% vulvovaginal GVHD in adult
patients who attended the clinic, similar to the incidence described in the literature.
The data on VV-GVHD in the literature refers mainly to adult women. As gynecological
examination and follow-up is not done routinely in girls and adolescents who are not sexually
active, the incidence and characteristics of VV-GVHD in girls and adolescents who underwent
HSCT is unknown.
Methods:
Patients who underwent allogeneic HSCT before the age of 18, who are 18 years or older at the
time of the study and who are alive will be invited to participate in the study. Those who
will be willing to participate will complete questionnaires and undergo physical and
gynecological examination. At a single appointment, data will be acquired regarding: age,
time from transplantation, current medical status, medications,hormonal status,marital
status, sexual function and fertility (pregnancies and deliveries), assessment of sexual
development by a pediatric endocrinologist regarding Tunner stages,data regarding possible
vulvovaginal involvement, presence and scoring of GVHD in other organs and assessment of
patients' well being using the FACT-BMT score.
In order to assess engraftment and degree of chimerism, donor and host-specific DNA markers,
using male and female amelogenine gene PCR bands and by STR-PCR assay will be done.
Gynecological exam: in case the patient is sexually active, a complete vulvovaginal exam
using a speculum, bimanual exam and transvaginal ultrasound will be done. In case the patient
never had sexual intercourse, only external (vulvar) exam and abdominal ultrasound exam will
be done.
On exam, the following aspects will be evaluated: vulvar anatomy, vaginal examination for
adhesions, fibrosis or stenosis. Vaginal exam will include vaginal pH measurement, saline and
10% potassium hydroxide microscopy, evaluation for the presence of condylomas, Pap smear and
vaginal and cervical swab for HPV.
VV-GVHD will be defined according to clinical criteria, which include vulvovaginal anatomic
changes, mucosal erosion and inflammation.
Blood samples will be examined for:
hormonal status, measurements of blood Th1/Th2 cytokines and immunoglobulins levels.
Immune reconstitution will be evaluated by quantitative immune reconstitution done using
peripheral blood cells. The cells will be analyzed by flow cytometry using fluorescein
isothiocyanate antibodies for the absolute counts of various T cells sub populations, B
cells, NK and NKT cells.
Additional data regarding age at transplantation, menarchal status at transplantation, sexual
activity status at time of transplantation, diagnosis, donor relation, source of cells,
number of cells infused, protocol, conditioning regimen, immunosuppressive prophylaxis and
occurrence of GVHD in other organs will be acquired by anamnesis and from the patients'
files.
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