2026-04-27T15:10:03Zhttps://uvadoc.uva.es/oai/requestoai:uvadoc.uva.es:10324/61002025-03-03T10:20:11Zcom_10324_32522com_10324_952com_10324_894com_10324_43677com_10324_954com_10324_1134com_10324_931col_10324_32523col_10324_43678col_10324_1213
Ganfornina Álvarez, María Dolores
Pérez García, María Teresa
Gutiérrez, Gabriel
Miguel Velado, Eduardo
López López, José Ramón
Marín, Antonio
Sánchez Romero, Diego
González Martínez, Constancio
2014-09-19T16:44:20Z
2015-09-19T23:40:08Z
2005
Journal of Physiology, 2005, vol. 566, n. 2, p. 491-503
0022-3751
http://uvadoc.uva.es/handle/10324/6100
10.1113/jphysiol.2005.088815
491
2
503
Journal of Physiology
566
The carotid body (CB) is an arterial chemoreceptor, bearing specialized type I cells that respond
to hypoxia by closing specific K+ channels and releasing neurotransmitters to activate sensory
axons. Despitehaving detailed informationonthe electricalandneurochemicalchangestriggered
by hypoxia in CB, the knowledge of the molecular components involved in the signalling cascade
of the hypoxic response is fragmentary. This study analyses the mouse CB transcriptional
changes in response to low PO2 by hybridization to oligonucleotide microarrays. The transcripts
were obtained from whole CBs after mice were exposed to either normoxia (21% O2),
or physiological hypoxia (10% O2) for 24 h. The CB transcriptional profiles obtained under
these environmental conditions were subtracted fromthe profile of control non-chemoreceptor
adrenal medulla extracted from the same animals. Given the common developmental origin of
these two organs, they share many properties but differ specifically in their response to O2. Our
analysis revealed 751 probe sets regulated specifically in CB under hypoxia (388 up-regulated
and 363 down-regulated). These results were corroborated by assessing the transcriptional
changesof selectedgenesunderphysiologicalhypoxiawithquantitativeRT-PCR.Ourmicroarray
experiments revealed a number of CB-expressed genes (e.g. TH, ferritin and triosephosphate
isomerase) that were known to change their expression under hypoxia. However, we also found
novel genes that consistently changed their expression under physiological hypoxia. Among
them, a group of ion channels show specific regulation in CB: the potassium channels Kir6.1 and
Kcnn4 are up-regulated, while the modulatory subunit Kcnab1 is down-regulated by low PO2
levels.
eng
info:eu-repo/semantics/embargoedAccess
Genética
Comparative gene expression profile of mouse carotid body and adrenal medulla under physiological hypoxia
info:eu-repo/semantics/article