TY - JOUR
T1 - Expression of the dominant negative retinoid receptor, RAR403, alters telencephalic progenitor proliferation, survival, and cell fate specification
AU - Rajaii, Fatemeh
AU - Bitzer, Zachary T.
AU - Xu, Qing
AU - Sockanathan, Shanthini
N1 - Funding Information:
We thank S.J. Ji and B.Q. Zhuang for assistance with motor neuron analyses; S. Lawson for technical help; T.M. Jessell for Islet1:Cre mice, antibodies and generation of R26 RAR403 mice with B. Han and M. Mendelson; C. Mendelsohn and J. Rossant for RARE-hsp68LacZ mice; S. Anderson, G. Fishell, J. Nathans, V. Pachnis, H.J. Song, P. Soriano and B.G. Novitch for reagents. We thank S. Anderson, N. Gaiano, E. Hess, A. Kolodkin, B.Q. Zhuang, M. Rutlin, and P. Sabharwal for comments and scientific discussions. This work was supported by NARSAD, the March of Dimes, and a Klingenstein fellowship awarded to S.S. F.R. was supported by the NIH Medical Scientist Training Program.
PY - 2008/4/15
Y1 - 2008/4/15
N2 - Retinoic acid (RA) signaling plays critical roles in diverse cellular processes during nervous system development. In mouse models, the roles for RA signals in telencephalic development remain unclear, partly because of the ambiguity of RA telencephalic sources after E8.75. Here, we have developed a genetic approach that utilizes Cre-lox technology to conditionally express a potent dominant negative retinoid receptor, RAR403, in vivo. This approach blocks RA signaling pathways at the receptor level, enabling the disruption of RA signals in contexts in which the RA source is unknown. RAR403 expression throughout the developing telencephalon causes pronounced hypoplasia resulting from defective proliferation in dorsal telencephalic progenitors and extensive cell death. Furthermore, Nkx2.1+ progenitors in the medial ganglionic eminence (MGE) are misspecified such that they acquire a subset of lateral ganglionic eminence (LGE)-specific properties at the expense of MGE fates. This genetic approach reveals new roles for RA signaling in telencephalic proliferation, survival and fate specification, and underscores its utility in investigating the function of retinoid signaling pathways throughout peri- and postnatal development.
AB - Retinoic acid (RA) signaling plays critical roles in diverse cellular processes during nervous system development. In mouse models, the roles for RA signals in telencephalic development remain unclear, partly because of the ambiguity of RA telencephalic sources after E8.75. Here, we have developed a genetic approach that utilizes Cre-lox technology to conditionally express a potent dominant negative retinoid receptor, RAR403, in vivo. This approach blocks RA signaling pathways at the receptor level, enabling the disruption of RA signals in contexts in which the RA source is unknown. RAR403 expression throughout the developing telencephalon causes pronounced hypoplasia resulting from defective proliferation in dorsal telencephalic progenitors and extensive cell death. Furthermore, Nkx2.1+ progenitors in the medial ganglionic eminence (MGE) are misspecified such that they acquire a subset of lateral ganglionic eminence (LGE)-specific properties at the expense of MGE fates. This genetic approach reveals new roles for RA signaling in telencephalic proliferation, survival and fate specification, and underscores its utility in investigating the function of retinoid signaling pathways throughout peri- and postnatal development.
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U2 - 10.1016/j.ydbio.2008.01.041
DO - 10.1016/j.ydbio.2008.01.041
M3 - Article
C2 - 18329011
AN - SCOPUS:41149131597
SN - 0012-1606
VL - 316
SP - 371
EP - 382
JO - Developmental biology
JF - Developmental biology
IS - 2
ER -