Clinical, Cellular, and Molecular Investigation Into Oculocutaneous Albinism
| Status: | Recruiting |
|---|---|
| Conditions: | Other Indications, Ocular, Dermatology |
| Therapuetic Areas: | Dermatology / Plastic Surgery, Ophthalmology, Other |
| Healthy: | No |
| Age Range: | 1 - 80 |
| Updated: | 3/14/2019 |
| Start Date: | December 11, 2008 |
| Contact: | David R Adams, M.D. |
| Email: | david.adams@nih.gov |
| Phone: | (301) 402-6435 |
Clinical, Cellular, and Molecular Investigations Into Oculocutaneous Albinism
Oculocutaneous albinism (OCA) is a term used to describe inherited forms of hypopigmentation
associated with 1) variable levels of cutaneous hypopigmentation, ocular hypopigmentation,
and visual deficits, and 2) involvement of both of the major developmental types of pigmented
cells, i.e., melanocytes and retinal pigment epithelium. OCA that affects only
usually-pigmented tissues is termed isolated OCA. There are currently seven albinism types
(OCA-1 to OCA-7). With the exception of OCA-5, eash is associated with a specific gene and is
inherited in an autosomal recessive manner OCA-5 is a proposed type of albinism associated
with the chromosomal location 4q24. OCA-1 results from defects in the enzyme tyrosinase,
which catalyzes the rate-limiting step in melanin synthesis. The precise functions of the
remaining genes are not yet fully understood, but several may be associated with the
regulation of pH in the subcellular organelle where melanin in manufactured-the melanosome.
The majority of persons with OCA have two pathogenic mutations identified in a known
OCA-causing gene, but a substantial minority to not. Ocular albinism (OA) is an X-linked
disorder caused by mutations in the GPR143 gene. It affects the eye in a manner similar to
OCA, but has minimal or no skin manifestations.
In this protocol, we have four major goals:
1. To clinically and comprehensively characterize OCA types 1 - 7, and OA, with respect to
the degree of hypopigmentation, genetic mutations, extent of ocular involvement, and
longitudinal variation.
2. To use study participants cultured melanocytes to study pigment biology, variability in
pigment formation related to genotype, and response to proposed treatments. Some of this
work will be performed collaboratively.
3. To recruit study participants with hypopigmentation not due to known albinismcausing
genes.
4. To evaluate methods of quantifying eye pigmentation, skin pigmentation and other
clinical parameters that may be usable as outcome measures in future treatment studies.
To achieve those goals, we will perform clinical evaluations of persons with OCA and OA at
the NIH Clinical Center; obtain cultured cells, plasma, serum and urine for future studies;
and, perform mutation analysis on known OCA and/or OA genes and search for other genes
responsible for albinism. Routine admissions will last 3 - 4 days and occur every 2 - 3
years.
associated with 1) variable levels of cutaneous hypopigmentation, ocular hypopigmentation,
and visual deficits, and 2) involvement of both of the major developmental types of pigmented
cells, i.e., melanocytes and retinal pigment epithelium. OCA that affects only
usually-pigmented tissues is termed isolated OCA. There are currently seven albinism types
(OCA-1 to OCA-7). With the exception of OCA-5, eash is associated with a specific gene and is
inherited in an autosomal recessive manner OCA-5 is a proposed type of albinism associated
with the chromosomal location 4q24. OCA-1 results from defects in the enzyme tyrosinase,
which catalyzes the rate-limiting step in melanin synthesis. The precise functions of the
remaining genes are not yet fully understood, but several may be associated with the
regulation of pH in the subcellular organelle where melanin in manufactured-the melanosome.
The majority of persons with OCA have two pathogenic mutations identified in a known
OCA-causing gene, but a substantial minority to not. Ocular albinism (OA) is an X-linked
disorder caused by mutations in the GPR143 gene. It affects the eye in a manner similar to
OCA, but has minimal or no skin manifestations.
In this protocol, we have four major goals:
1. To clinically and comprehensively characterize OCA types 1 - 7, and OA, with respect to
the degree of hypopigmentation, genetic mutations, extent of ocular involvement, and
longitudinal variation.
2. To use study participants cultured melanocytes to study pigment biology, variability in
pigment formation related to genotype, and response to proposed treatments. Some of this
work will be performed collaboratively.
3. To recruit study participants with hypopigmentation not due to known albinismcausing
genes.
4. To evaluate methods of quantifying eye pigmentation, skin pigmentation and other
clinical parameters that may be usable as outcome measures in future treatment studies.
To achieve those goals, we will perform clinical evaluations of persons with OCA and OA at
the NIH Clinical Center; obtain cultured cells, plasma, serum and urine for future studies;
and, perform mutation analysis on known OCA and/or OA genes and search for other genes
responsible for albinism. Routine admissions will last 3 - 4 days and occur every 2 - 3
years.
Oculocutaneous albinism (OCA) is a term used to describe inherited forms of hypopigmentation
associated with 1) variable levels of cutaneous hypopigmentation, ocular hypopigmentation,
and visual deficits, and 2) involvement of both of the major developmental types of pigmented
cells, i.e., melanocytes and retinal pigment epithelium. OCA that affects
only usually-pigmented tissues is termed isolated OCA. There are currently seven albinism
types (OCA-1 to OCA-7). With the exception of OCA-5, eash is associated with a specific
gene and is inherited in an autosomal recessive manner (see Table 1). OCA-5 is a proposed
type of albinism associated with the chromosomal location 4q24. OCA-1 results from defects
in the enzyme tyrosinase, which catalyzes the rate-limiting step in melanin synthesis. The
precise functions of the remaining genes are not yet fully understood, but several may be
associated with the regulation of pH in the subcellular organelle where melanin in
manufactured the melanosome. The majority of persons with OCA have two pathogenic
mutations identified in a known OCA-causing gene, but a substantial minority to not. Ocular
albinism (OA) is an X-linked disorder caused by mutations in the GPR143 gene. It affects the
eye in a manner similar to OCA, but has minimal or no skin manifestations.
In this protocol, we have four major goals:
1. To clinically and comprehensively characterize OCA types 1 7, and OA, with respect
to the degree of hypopigmentation, genetic mutations, extent of ocular involvement,
and longitudinal variation.
2. To use study participants cultured melanocytes to study pigment biology, variability
in pigment formation related to genotype, and response to proposed treatments. Some
of this work will be performed collaboratively
3. To recruit study participants with hypopigmentation not due to known albinismcausing
genes.
4. To evaluate methods of quantifying eye pigmentation, skin pigmentation and other
clinical parameters that may be usable as outcome measures in future treatment studies.
To achieve those goals, we will perform clinical evaluations of persons with OCA and OA at
the NIH Clinical Center; obtain cultured cells, plasma, serum and urine for future studies;
and,
perform mutation analysis on known OCA and/or OA genes and search for other genes
responsible for albinism. Routine admissions will last 3 - 4 days and occur every 2 - 3
years.
associated with 1) variable levels of cutaneous hypopigmentation, ocular hypopigmentation,
and visual deficits, and 2) involvement of both of the major developmental types of pigmented
cells, i.e., melanocytes and retinal pigment epithelium. OCA that affects
only usually-pigmented tissues is termed isolated OCA. There are currently seven albinism
types (OCA-1 to OCA-7). With the exception of OCA-5, eash is associated with a specific
gene and is inherited in an autosomal recessive manner (see Table 1). OCA-5 is a proposed
type of albinism associated with the chromosomal location 4q24. OCA-1 results from defects
in the enzyme tyrosinase, which catalyzes the rate-limiting step in melanin synthesis. The
precise functions of the remaining genes are not yet fully understood, but several may be
associated with the regulation of pH in the subcellular organelle where melanin in
manufactured the melanosome. The majority of persons with OCA have two pathogenic
mutations identified in a known OCA-causing gene, but a substantial minority to not. Ocular
albinism (OA) is an X-linked disorder caused by mutations in the GPR143 gene. It affects the
eye in a manner similar to OCA, but has minimal or no skin manifestations.
In this protocol, we have four major goals:
1. To clinically and comprehensively characterize OCA types 1 7, and OA, with respect
to the degree of hypopigmentation, genetic mutations, extent of ocular involvement,
and longitudinal variation.
2. To use study participants cultured melanocytes to study pigment biology, variability
in pigment formation related to genotype, and response to proposed treatments. Some
of this work will be performed collaboratively
3. To recruit study participants with hypopigmentation not due to known albinismcausing
genes.
4. To evaluate methods of quantifying eye pigmentation, skin pigmentation and other
clinical parameters that may be usable as outcome measures in future treatment studies.
To achieve those goals, we will perform clinical evaluations of persons with OCA and OA at
the NIH Clinical Center; obtain cultured cells, plasma, serum and urine for future studies;
and,
perform mutation analysis on known OCA and/or OA genes and search for other genes
responsible for albinism. Routine admissions will last 3 - 4 days and occur every 2 - 3
years.
- INCLUSION CRITERIA:
Patients will be screened by requesting copies of the following materials at the time they
contact the program:
1. An indication of ethnic background by the potential participant, which may be unknown
.
2. Photographs of the potential participant that give an indication of skin
complexion/pigmentation and undyed hair color (if available).
3. Ophthalmology or other visual specialist records documenting visual exam
characteristics, potentially including iris transillumination, visual evoked potential
and or characteristic eye findings (if available).
4. Genetic testing results (if available).
EXCLUSION CRITERIA:
Exclusion from the study will be made based on one or more of the following criteria:
1. Significant evidence that the potential participant has either OCA1A or OCA2 with a
typical presentation, AND has an ethnic background that is wellrepresented in the
current study (proportion in study exceeding the proportion in the United States
population).
The rationale for this exclusion is that: 1) from a biologicaland clinicalresearch
perspective, we have an adequate number of OCA1A/
OCA2 cases in the current study population; and 2) that, despite this, persons with
ethnicities that are underrepresented in the study may inform our understanding of
populationlevel molecular patterns in OCA1A/ OCA2 and cultural implications of
albinism.
2. Persons who are under 1 year of age. This exclusion occurs because there is no urgency
for a very early evaluation. Also, the Clinical Center staff and resources are more
suited for the care of older children.
3. Persons who are too sick to travel safely to the NIH Clinical Center.
4. A judgment by the principal investigator that clinical resources are not available to
enroll additional patients at any given time.
5. Persons who are currently incarcerated.
6. Adults who are incompetent to consent to the protocol.
7. Persons who have been diagnosed with a known nonoculocutaneous disorder of
hypopigmentation such as HemanskyPudlak Syndrome, ChediakHigashi Syndrome, or
Griscelli Syndrome.
8. Persons who have been diagnosed with a known disorder of focal hypopigmentation such
as Waardenburg syndrome.
We found this trial at
1
site
9000 Rockville Pike
Bethesda, Maryland 20892
Bethesda, Maryland 20892
Phone: 800-411-1222
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