Sebaceous carcinomas (SeC) are cutaneous malignancies that, in rare cases, metastasize and prove fatal. Here we report whole-exome sequencing on 32 SeC, revealing distinct mutational classes that explain both cancer ontogeny and clinical course. A UV-damage signature predominates in 10/32 samples, while nine show microsatellite instability (MSI) profiles. UV-damage SeC exhibited poorly differentiated, infiltrative histopathology compared to MSI signature SeC (p = 0.003), features previously associated with dissemination. Moreover, UV-damage SeC transcriptomes and anatomic distribution closely resemble those of cutaneous squamous cell carcinomas (SCC), implicating sun-exposed keratinocytes as a cell of origin. Like SCC, this UV-damage subclass harbors a high somatic mutation burden with >50 mutations per Mb, predicting immunotherapeutic response. In contrast, ocular SeC acquires far fewer mutations without a dominant signature, but show frequent truncations in the ZNF750 epidermal differentiation regulator. Our data exemplify how different mutational processes convergently drive histopathologically related but clinically distinct cancers.
The barrier epithelia of the cornea and retina control drug and nutrient
access to various compartments of the human eye. While ocular transporters are
likely to play a critical role in homeostasis and drug delivery, little is known
about their expression, localization and function. In this study, the mRNA
expression levels of 445 transporters, metabolic enzymes, transcription factors
and nuclear receptors were profiled in five regions of the human eye: cornea,
iris, ciliary body, choroid and retina. Through RNA expression profiling and
immunohistochemistry, several transporters were identified as putative targets
for drug transport in ocular tissues. Our analysis identified
SLC22A7 (OAT2), a carrier for the anti-viral drug,
acyclovir, in the corneal epithelium, in addition to ABCG2
(BCRP), an important xenobiotic efflux pump, in retinal nerve fibers and the
retinal pigment epithelium. Collectively, our results provide an understanding
of the transporters that serve to maintain ocular homeostasis and which may be
potential targets for drug delivery to deep compartments of the eye.
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