Pain Clinical Trial
Official title:
Biochemical and Genetic Mechanisms for Etiology of Sickle Cell Pain
Background:
- Sickle cell disease often causes crises, with episodes of pain. Many people with sickle
cell disease also have pain between crises. Inflammation is an important part of sickle cell
pain. It may be related to levels of nitric oxide. Nitric oxide is a gas in the body that
helps relax blood vessels and may be related to the pain from sickle cell disease.
Researchers want to study the relationship between blood levels of nitric oxide and pain in
people with sickle cell disease. Researchers also want to study how certain genes express
themselves related to sickle cell pain.
Objectives:
- To collect blood samples and other genetic expression information to study sickle cell pain
and its relation to nitric oxide levels in the blood.
Eligibility:
- People at least 18 years of age who have sickle cell disease.
- Healthy volunteers at least 18 years of age.
Design:
- This study requires a screening visit and four study visits scheduled 1 week apart. Each
visit will last about 1 hour.
- Participants will be screened with a medical history and physical exam. They will
complete questionnaires about pain levels (if any). They will also provide blood samples
for genetic and other testing.
- Participants will have a breath test to see how much nitric oxide they exhale. They will
also have a test of their ability to detect small changes in temperature and touch.
- Participants will keep a diary to record daily pain levels and pain medicines taken.
They will write down what they eat to track foods that contain nitrates (such as meats
like ham and bacon and vegetables like beets and spinach).
- At each of the four study visit, participants will bring the pain diary, provide blood
samples, and have breath nitric oxide tests.
Sickle cell disease is a systemic disorder whose proximate cause is a mutation in the
beta-globin chain of hemoglobin. Although it is characterized by differing degrees and
patterns of clinical manifestations, its major features include severe episodes of pain. The
sickle cell pain crisis is one of the most typical characteristics of this disease and pain
associated with crisis is reported to be more intense than other types of clinical pain by
those with sickle cell disease and displays both nociceptive and neuropathic qualities. Pain
in sickle cell disease is more widely experienced and poorly managed than previously
considered. In one community sample, more than 50 percent of the patients reported
experiencing pain on more than half the days of the study period. Painful crisis consist of
pain experienced in different areas of the body, typically in the extremities, back, abdomen
and chest and some studies suggest that patients experience prodromal or pre-crisis phases of
their pain, some of which last up to 24 hours before developing the typical features of a
pain crisis. The nature of pain experience in patients with sickle cell disease is not well
documented nor are the mechanisms of sickle cell pain well understood.
Objectives: The first objective of the study is to characterize genetic expression data of
sickle cell disease and matched controls at weekly time points over a 4 week period. The
second objective is to measure levels of exhaled Nitric Oxide (eNO) and other biomarkers in
sickle cell patients and in matched controls over the same time points. The third objective
is to evaluate experimental pain perception in both groups.
Population: By stratifying patients by pain level, this study will recruit sickle cell
patients with a range of symptom severity (N=45) and sex-, race-, ethnicity and age-matched
controls (N=45) without sickle cell trait from the NIH Patient Recruitment and Referral
Service.
Design: This is a prospective, exploratory study of steady state and acute pain phase in
sickle cell patients. Participants will undergo evaluations (eNO and blood collection) during
weekly clinic visits and keep a pain diary for 4 weeks after the first visit. All
participants will also undergo one session of quantitative sensory testing.
Importance: The purpose of this study is to improve the understanding of the biochemical and
molecular genetic mechanisms associated with sickle cell pain by characterizing the
transcriptome of sickle cell disease during steady state and pain phases. It is hypothesized
that analysis of the transcriptome will result in a panel of biomarkers that correlate with
the severity level of pain and perhaps signal the onset of a painful episode. The successful
elucidation of these relationships may identify novel targets for intervention leading to
attenuation of sickle cell pain, improved treatment and less impact on quality of life and
functional status.
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