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CRISPR knockouts of pmela and pmelb engineered a golden tilapia by regulating relative pigment cell abundance
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Abstract
Premelanosome protein
(pmel)
is a key gene for melanogenesis in vertebrates. Mutations in this gene are responsible for white plumage in chicken, but its role in pigmentation of fish remains to be demonstrated. In this study we found that most fishes have two
pmel
genes arising from the teleost-specific whole genome duplication. Both
pmela and pmelb
were expressed at high levels in the eyes and skin of Nile tilapia. We mutated both genes in tilapia using CRISPR/Cas9 gene editing. Homozygous mutation of
pmela
resulted in yellowish body color with weak vertical bars and a hypo-pigmented retinal pigment epithelium (RPE) due to significantly reduced number and size of melanophores. In contrast, we observed an increased number and size of xanthophores in mutants compared to wild-type fish. Homozygous mutation of
pmelb
resulted in a similar, but milder phenotype than
pmela
-/-
mutants, without effects on RPE pigmentation. Double mutation of
pmela
and
pmelb
resulted in loss of additional melanophores compared to the
pmela
-/-
mutants, and also an increase in the number and size of xanthophores, producing a strong golden body color without bars in the trunk. The RPE pigmentation of
pmela
-/-
;pmelb
-/-
was similar to
pmela
-/-
mutants, with much less pigmentation than
pmelb
-/-
mutants and wild-type fish. Taken together, our results indicate that, while both
pmel
genes are important for the formation of body color in tilapia,
pmela
plays a more important role than
pmelb
. To our knowledge, this is the first report on mutation of
pmelb
or both
pmela;pmelb
in fish. Studies on these mutants suggest new strategies for breeding golden tilapia, and also provide a new model for studies of
pmel
function in vertebrates.
Author Summary
Melanophores, the most common pigment cell type, have been studied for nearly 150 years. Many genes are involved in melanoblast migration, melanophore differentiation, and melanin biosynthesis.
Pmel
is fundamental for melanosome development by directing melanin biosynthesis and melanosome phase transition. Specifically, PMEL can form a fibrillar structure within the melanosome upon which melanin is deposited. We identified two
pmel
genes in Nile tilapia arising from the teleost-specific whole genome duplication. Disruption of either
pmela
or
pmelb
in tilapia leads to significant hypo-pigmentation. PMEL disrupted fish showed not only a reduction in melanin and tiny melanophores, but also a significant increase in the number of xanthophores, and even guanine-filled melanophores, which led to a golden tilapia with hypo-pigmented RPE. Our study confirmed the role of
pmel
in melanin biosynthesis and maturation, and also highlighted its effects on melanophore number and size. These results provide new insights into pigment cell biology and will help us better understand the mechanisms of color patterning in teleosts. Knockout of both
pmela
and
pmelb
provide a new strategy for engineering a golden tilapia, which might provide a foundation for developing new strains in the tilapia industry.
Title: CRISPR knockouts of
pmela
and
pmelb
engineered a golden tilapia by regulating relative pigment cell abundance
Description:
Abstract
Premelanosome protein
(pmel)
is a key gene for melanogenesis in vertebrates.
Mutations in this gene are responsible for white plumage in chicken, but its role in pigmentation of fish remains to be demonstrated.
In this study we found that most fishes have two
pmel
genes arising from the teleost-specific whole genome duplication.
Both
pmela and pmelb
were expressed at high levels in the eyes and skin of Nile tilapia.
We mutated both genes in tilapia using CRISPR/Cas9 gene editing.
Homozygous mutation of
pmela
resulted in yellowish body color with weak vertical bars and a hypo-pigmented retinal pigment epithelium (RPE) due to significantly reduced number and size of melanophores.
In contrast, we observed an increased number and size of xanthophores in mutants compared to wild-type fish.
Homozygous mutation of
pmelb
resulted in a similar, but milder phenotype than
pmela
-/-
mutants, without effects on RPE pigmentation.
Double mutation of
pmela
and
pmelb
resulted in loss of additional melanophores compared to the
pmela
-/-
mutants, and also an increase in the number and size of xanthophores, producing a strong golden body color without bars in the trunk.
The RPE pigmentation of
pmela
-/-
;pmelb
-/-
was similar to
pmela
-/-
mutants, with much less pigmentation than
pmelb
-/-
mutants and wild-type fish.
Taken together, our results indicate that, while both
pmel
genes are important for the formation of body color in tilapia,
pmela
plays a more important role than
pmelb
.
To our knowledge, this is the first report on mutation of
pmelb
or both
pmela;pmelb
in fish.
Studies on these mutants suggest new strategies for breeding golden tilapia, and also provide a new model for studies of
pmel
function in vertebrates.
Author Summary
Melanophores, the most common pigment cell type, have been studied for nearly 150 years.
Many genes are involved in melanoblast migration, melanophore differentiation, and melanin biosynthesis.
Pmel
is fundamental for melanosome development by directing melanin biosynthesis and melanosome phase transition.
Specifically, PMEL can form a fibrillar structure within the melanosome upon which melanin is deposited.
We identified two
pmel
genes in Nile tilapia arising from the teleost-specific whole genome duplication.
Disruption of either
pmela
or
pmelb
in tilapia leads to significant hypo-pigmentation.
PMEL disrupted fish showed not only a reduction in melanin and tiny melanophores, but also a significant increase in the number of xanthophores, and even guanine-filled melanophores, which led to a golden tilapia with hypo-pigmented RPE.
Our study confirmed the role of
pmel
in melanin biosynthesis and maturation, and also highlighted its effects on melanophore number and size.
These results provide new insights into pigment cell biology and will help us better understand the mechanisms of color patterning in teleosts.
Knockout of both
pmela
and
pmelb
provide a new strategy for engineering a golden tilapia, which might provide a foundation for developing new strains in the tilapia industry.
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CRISPR Knockouts of
pmela
and
pmelb
Engineered a Golden Tilapia by Regulating Relative Pigment Cell Abundance
CRISPR Knockouts of
pmela
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pmelb
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