Suppressed NFAT-dependent VEGFR1 expression and constitutive VEGFR2 signaling in infantile hemangioma
21/10/2008
Infantile hemangiomas are localized and rapidly
growing regions of disorganized angiogenesis. We show
that expression of vascular endothelial growth factor
receptor-1 (VEGFR1) in hemangioma endothelial cells
(hemECs) and hemangioma tissue is markedly reduced
compared to controls. Low VEGFR1 expression in hemECs
results in VEGF-dependent activation of VEGFR2 and
downstream signaling pathways. In hemECs,
transcription of the gene encoding VEGFR1 (FLT1) is
dependent on nuclear factor of activated T cells
(NFAT). Low VEGFR1 expression in hemECs is caused by
reduced activity of a pathway involving beta1
integrin, the integrin-like receptor tumor
endothelial marker-8 (TEM8), VEGFR2 and NFAT. In a
subset of individuals with hemangioma, we found
missense mutations in the genes encoding VEGFR2 (KDR)
and TEM8 (ANTXR1). These mutations result in
increased interactions among VEGFR2, TEM8 and beta1
integrin proteins and in inhibition of integrin
activity. Normalization of the constitutive VEGFR2
signaling in hemECs with soluble VEGFR1 or antibodies
that neutralize VEGF or stimulate beta1 integrin
suggests that local administration of these or
similar agents may be effective in hemangioma
treatment.
Nature Medicine
Published online: 19 October 2008 | doi:10.1038/nm.1877
Nature Medicine
Published online: 19 October 2008 | doi:10.1038/nm.1877
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Natural selection of FLT1 alleles and their association with malaria resistance in utero
09/09/2008
Placental
malaria (PM) caused by Plasmodium falciparum
contributes significantly to infant mortality in
sub-Saharan Africa and is associated with pregnancy
loss. We hypothesized that fetal genes that modify PM
would be associated with fetal fitness. During PM,
placental trophoblasts produce soluble fms-like
tyrosine kinase 1 (sFlt1), also known as soluble VEGF
receptor 1, an angiogenesis inhibitor associated with
preeclampsia. Here we present a study examining the
genotype of the fms-related tyrosine kinase 1 (FLT1)
3′ UTR in Tanzanian mother–infant pairs. First-time
mothers suffer the most PM, and newborn FLT1 genotype
distribution differed by birth order, with newborns
of first-time mothers outside of Hardy–Weinberg
equilibrium (HWE) during peak PM season. Among
first-time but not other mothers, maternal FLT1
genotype was associated with a history of prior
pregnancy loss. During PM, newborn FLT1 genotype was
associated with low birth weight and placental
inflammatory gene expression. FLT1 genotype was also
associated with Flt1 levels among study subjects and
in vitro. Thus, FLT1 variants confer fetal fitness in
utero and are associated with the maternal immune
response during PM. This indicates that FLT1 is under
natural selection in a malaria endemic area and that
human exposure to malaria can influence the
evolutionary genetics of the maternal-fetal
relationship.
PNAS published September 8, 2008, doi:10.1073/pnas.0803657105
PNAS published September 8, 2008, doi:10.1073/pnas.0803657105