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Genetic analysis of rab7 mutants in zebrafish
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Abstract
Vascular network formation requires the fusion of newly formed blood vessels and the emergence of a patent lumen between the newly established connections so that blood flow can start. Lumen formation has been shown to depend on the late endosomal/lysosomal pathway in various organs of animal tubular systems. Here, we identified a late endosomal/lysosomal vesicular fraction (Rab7/Lamp2) in early zebrafish angiogenic sprouts, which appears to contribute to apical membrane growth during lumen formation. To study the effect of the late endocytic pathway on vascular development, we generated mutant alleles for all three
rab7
genes in zebrafish (
rab7a, rab7ba, rab7bb
). All
rab7
genes are expressed in wild-type zebrafish and we did not detect any compensatory effects by the other
rab7
isoforms in single knockout mutants, which were all viable. Only the triple mutant was lethal suggesting some functional redundancy. However, the different
rab7
isoforms fulfil also at least partially independent functions because eggs laid from mothers lacking two
rab7
(
rab7a and/or rab7bb
). showed reduced survival and contained enlarged yolk granules, suggesting maternal contribution of these two
rab7
. Finally, we observed minor effects on lumen formation in embryos which still express one copy of
rab7
. Our results support the notion that the late endocytic/lysosomal compartment contributes to lumen expansion.
Title: Genetic analysis of
rab7
mutants in zebrafish
Description:
Abstract
Vascular network formation requires the fusion of newly formed blood vessels and the emergence of a patent lumen between the newly established connections so that blood flow can start.
Lumen formation has been shown to depend on the late endosomal/lysosomal pathway in various organs of animal tubular systems.
Here, we identified a late endosomal/lysosomal vesicular fraction (Rab7/Lamp2) in early zebrafish angiogenic sprouts, which appears to contribute to apical membrane growth during lumen formation.
To study the effect of the late endocytic pathway on vascular development, we generated mutant alleles for all three
rab7
genes in zebrafish (
rab7a, rab7ba, rab7bb
).
All
rab7
genes are expressed in wild-type zebrafish and we did not detect any compensatory effects by the other
rab7
isoforms in single knockout mutants, which were all viable.
Only the triple mutant was lethal suggesting some functional redundancy.
However, the different
rab7
isoforms fulfil also at least partially independent functions because eggs laid from mothers lacking two
rab7
(
rab7a and/or rab7bb
).
showed reduced survival and contained enlarged yolk granules, suggesting maternal contribution of these two
rab7
.
Finally, we observed minor effects on lumen formation in embryos which still express one copy of
rab7
.
Our results support the notion that the late endocytic/lysosomal compartment contributes to lumen expansion.
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