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1 solated from rodents at the end of the first postnatal week.
2 s detectable paternal Ube3a beyond the first postnatal week.
3 a similar length toward the end of the first postnatal week.
4 antly increase in the heart during the first postnatal week.
5 s calcium action potentials during the first postnatal week.
6 the developing cortical plate in the second postnatal week.
7 ression levels were highest during the first postnatal week.
8 - 0.14 cell/40-mum section during the second postnatal week.
9 ion and myelination recover during the first postnatal week.
10 ype levels in the brain beginning the second postnatal week.
11 irth and are fully established by the second postnatal week.
12 nd continuing to do so well after the eighth postnatal week.
13 tinguish gamma-from alpha-MNs into the third postnatal week.
14 ed, GDNF-independent signal during the first postnatal week.
15 creased in the Ts65Dn mice during the second postnatal week.
16 e SO in vestibular hair cells over the first postnatal week.
17 l cortex becomes prominent during the second postnatal week.
18 e patterns by the end of the third or fourth postnatal week.
19 ge-matched controls at the end of the second postnatal week.
20 rent input and begin to die during the first postnatal week.
21 icotinic acetylcholine currents in the third postnatal week.
22 these synapses between the first and second postnatal week.
23 del-COMP triggers apoptosis during the first postnatal week.
24 recovery in beta2-/- mice during the second postnatal week.
25 1) to the SC is established during the first postnatal week.
26 ath of these animals near the end of the 2nd postnatal week.
27 rtical activity only by the end of the first postnatal week.
28 g a short window during the second and third postnatal week.
29 g and excitability decreasing into the third postnatal week.
30 icantly increased in diameter over the first postnatal week.
31 l coupling was decreasing, during the second postnatal week.
32 downregulate its expression during the first postnatal week.
33 and die because of seizures during the third postnatal week.
34 nscript and protein occurs during the second postnatal week.
35 postnatal week, but return during the second postnatal week.
36 by BAX-dependent apoptosis during the first postnatal week.
37 mature in the outer retina during the second postnatal week.
38 thood, with peak expression during the first postnatal week.
39 he AS-related theta rhythm during the second postnatal week.
40 frequency range (30-80 Hz) during the fourth postnatal week.
41 inputs relative to controls after the first postnatal week.
42 synaptic development beginning in the first postnatal week.
43 y 13, reaching maximal enrichment by the 3rd postnatal week.
44 activation and for survival beyond the first postnatal week.
45 eaching adult levels at the end of the third postnatal week.
46 he rest of embryogenesis and into the second postnatal week.
47 e neurological deficits and die in the third postnatal week.
48 occur significantly later, during the first postnatal week.
49 diated inputs to D1 SPNs, both in the second postnatal week.
50 d currents compared to wildtype in the third postnatal week.
51 , tonic NMDA current at the end of the first postnatal week.
52 ring development, until the end of the third postnatal week.
53 erent strata of CA3 in rats during the third postnatal week.
54 Pcdh19 and Ncdh expression during the first postnatal week.
55 rred mostly between the second and the third postnatal week.
56 ons and inhibitory interneurons in the first postnatal week.
57 of the deep cortical layers until the first postnatal week.
58 m thalamocortical afferents during the first postnatal week.
59 obtain adult-like features until the fourth postnatal week.
60 e apparent at embryonic day 18 and the first postnatal week.
61 olarizing potentials (GDPs) during the first postnatal week.
62 ons and inhibitory interneurons in the first postnatal week.
63 hat specifically targets L4 during the first postnatal week.
64 ntiate from retinal progenitors in the first postnatal week.
65 DSGCs at the beginning and end of the second postnatal week.
66 epithelia of ILDR1 null mice after the first postnatal week.
67 nditioning begins to emerge during the third postnatal week.
68 air cells degenerate rapidly after the first postnatal week.
69 tivity-dependent refinement during the first postnatal weeks.
70 ion of protein malnutrition during the first postnatal weeks.
71 elected brain regions during the first three postnatal weeks.
72 effect was smaller and confined to the first postnatal weeks.
73 s place almost entirely in the first several postnatal weeks.
74 rk activity, especially during the first two postnatal weeks.
75 lly during development, but die in the early postnatal weeks.
76 fiber inputs mature gradually over the first postnatal weeks.
77 but markedly increased during the first 2-3 postnatal weeks.
78 rain amoeboid microglia during the first two postnatal weeks.
79 in barrel cortex during the third and fourth postnatal weeks.
80 pment, and are active only for the first few postnatal weeks.
81 ly isolated from rats during the first three postnatal weeks.
82 xcitatory to inhibitory during the first two postnatal weeks.
83 and density of SMI-32(+) neurons around 2-5 postnatal weeks.
84 development, peaking in the first to second postnatal weeks.
85 re anatomical features until approximately 8 postnatal weeks.
86 cy and amplitude increase during the first 3 postnatal weeks.
87 l ganglion cells (RGCs) during the first two postnatal weeks.
88 s is transient, being limited to the first 3 postnatal weeks.
89 transiently express syt 2 during the first 2 postnatal weeks.
90 ses progressively increased over the first 2 postnatal weeks.
91 ity within neural circuits, during the first postnatal weeks.
92 Aergic to glycinergic within the first three postnatal weeks.
93 liculus does not change across the first two postnatal weeks.
94 ciceptive spinal activity in the first three postnatal weeks.
95 ses muscle calcium levels during the first 2 postnatal weeks.
96 etion was induced in OPCs during the first 2 postnatal weeks.
97 eased muscle calcium only during the first 2 postnatal weeks.
98 each their ventral destinations during first postnatal weeks.
99 ing in developing mouse cardiomyocytes after postnatal week 1, a time when the cells are no longer di
102 g1 mice but falls below control levels after postnatal week 12, approximately correlating with the on
105 in the photoreceptor outer nuclear layer at postnatal week 2 and highly disorganized outer segments
106 orn: selective block of afferent C fibers in postnatal week 2, using perisciatic injections of the ca
113 was noted at 5 months of age and as early as postnatal week 4 in the eyes of four BBS mouse model str
116 2 and highly disorganized outer segments by postnatal weeks 4 to 6 was observed in all four strains.
118 ivity unilaterally during a critical period [postnatal week 5 (PW5) to PW7] produces permanent contra
121 tivated M1 by muscimol microinfusion between postnatal weeks 5 and 7 to examine activity-dependent in
125 collected from embryonic day 12.5 (E12.5) to postnatal week 8 (W8), encompassing major developmental
127 In mice, this ability is lost in the first postnatal week, a period physiologically similar to thyr
128 inal development during the second and third postnatal weeks, a period that corresponds to human embr
129 ration of these tissues over the first three postnatal weeks, a time when the normal cortex expands a
130 ironment, becomes more evident with age (> 7 postnatal weeks), activity and stress, is gender specifi
131 postnatal week (juvenile ELE, P21-27), 6(th) postnatal week (adolescent ELE, P35-41), or 4(th)-6(th)
132 t expressed by interneurons until the second postnatal week after reaching the cortex, suggesting tha
133 Arbor remodeling begins during the second postnatal week, after migration to and dispersion within
134 nock-out mice, we show that during the first postnatal week, alpha-syn is not required for synapse fo
135 e and retarded growth starting at the second postnatal week and died on approximately postnatal day 2
136 NS in developing hepatocytes from the first postnatal week and increased DNA damage and hepatocellul
137 letion in hippocampal CA1 cells in the third postnatal week and later throughout the neocortex, brain
139 pressed in some VBN neurons during the first postnatal week and sharply declined over the second week
140 cortical inputs to SPNs emerge in the second postnatal week and that SPNs that receive superficial co
141 blished in the inner retina during the first postnatal week and that these systems subsequently matur
142 te that mouse microglia mature by the second postnatal week and to predict novel microglial functions
143 es of BG microglia emerged during the second postnatal week and were re-established following genetic
144 ed the retinal vasculogenesis in the first 2 postnatal weeks and impaired the angiogenesis triggered
145 dergoes profound regulation over the first 4 postnatal weeks and that these changes are correlated wi
146 y had achieved their adult-like anatomy by 4 postnatal weeks and were in a position to influence the
147 ) mitochondria become abnormal by the second postnatal week, and a majority of PNs die in the fourth
149 AVPV fibers reached the PVH during the first postnatal week, and fibers targeting the BSTp and LSv we
150 atal histaminergic innervation by the second postnatal week, and qRT-PCR shows transcripts for H(1),
151 in inner hair cells (IHCs) during the first postnatal week, and the pattern differs along the cochle
152 red CH formation and growth during the first postnatal week, and the phenotypes were exacerbated by f
153 n between VBN relay neurons during the first postnatal week, and then declined sharply during the sec
155 nsequences of inflammation during the second postnatal week are stunted dendrites of the cerebellum's
156 ed hippocampal gamma rhythm during the first postnatal week, as well as the emergence of the AS-relat
157 dendritic spine dynamics during the first 2 postnatal weeks, as immature filopodia are replaced by m
158 ha10-mediated transmission beyond the second postnatal week associated with abnormally persistent cho
159 ells decreases between the second and fourth postnatal week, at a time when PV cell synapse numbers i
160 ot altered in fmr1 KO mice until the 3rd-4th postnatal week, beyond this age it failed to develop fur
162 Neuronal number decreased during the first postnatal week but increased 2.5-fold over the next 3 we
163 of heightened arousal during the first three postnatal weeks but comes under inhibitory control in ra
164 dx1(Fl) mice were euglycemic for the first 2 postnatal weeks but showed moderate hyperglycemia from 3
165 ent LTP via H(3) receptors during the second postnatal week, but inhibits synaptic plasticity at late
166 ed retinal waves are absent during the first postnatal week, but return during the second postnatal w
167 itors significantly declines after the early postnatal weeks, but Foxj1-derived neurons in the OB per
168 e majority of PNs die in the fourth to fifth postnatal weeks, but the responsible molecules are unkno
169 clined almost eightfold during the first two postnatal weeks, but there were offsetting increases in
170 cerebellum occur primarily during the third postnatal week by both FISH and immunocytochemistry.
171 life exercise, specifically during the 4(th) postnatal week, can enable hippocampal memory, synaptic
172 mPFC neuron excitability during the first 2 postnatal weeks caused a premature differentiation of ol
174 at PVFSIs upregulate GluA4 during the second postnatal week coincident with increases in the AMPAR cl
175 gic inhibitory control emerges in the second postnatal week, coinciding with an expression switch fro
176 ces from immature rats (i.e. second to third postnatal weeks), compared to CA3 slices from adult rats
178 l period, in particular, prior to the fourth postnatal week, corresponding to stages in which VEGF in
180 showed previously that the end of the second postnatal week (days P11-15) represents a period of deve
182 sensorimotor reflex development in the first postnatal week followed by a degeneration of motor funct
183 showed a substantial increase until the 4th postnatal week followed by a further but moderate increa
184 V(E) ) significantly increased in the second postnatal week, followed by a progressive increase in V(
185 l and temporal cortices during the first two postnatal weeks following three episodes of status-epile
186 retinal waves are necessary during the first postnatal week for both proper distribution and eye-spec
188 inner nuclear layer at the end of the first postnatal week, from postnatal day (P) 5 to P9, after th
191 ion blocker, carbenoxolone, during the first postnatal week greatly diminished the functional similar
193 ernal separation (MS15) during the first 1-2 postnatal weeks has been shown to increase active matern
194 associated with male gender, older age (> 7 postnatal weeks), higher locomotor activity, daytime rec
196 integrity, increased at the end of the third postnatal week in association with increases in AMPAR re
197 sue anisotropy was measured during the first postnatal week in cortical regions, reflecting the under
202 of human pregnancy is equivalent to the 1st postnatal week in rodents; both are periods of active br
203 arameters remain unchanged through the first postnatal week in the absence of retinal waves, but quic
204 e excess inhibition at the end of the second postnatal week in Ts65Dn mice is not due to increases in
206 C) at birth, but develop over the first four postnatal weeks in different temporal patterns and also
208 els gradually increased over the first three postnatal weeks in the hippocampus, and remained stable
209 ial and neuronal subtypes during the first 3 postnatal weeks in the Long Evans and Sprague Dawley rat
211 tiated cells are eliminated in the first two postnatal weeks in these mice, resulting in a modest inc
213 already established by the first and second postnatal weeks, including different electrophysiologica
214 ion, axonal tracing in vivo during the first postnatal week indicates that immature mossy fibers exte
215 both inputs after the beginning of the third postnatal week, indicating that both types of inputs dis
216 , silent synapses persist through the second postnatal week, indicating that the maintenance of AMPA
217 eurons decreases between the third and fifth postnatal weeks, indicating a period of connection pruni
219 strongly suggests that the end of the second postnatal week is a critical period of development for b
220 erning of the barrel cortex during the first postnatal week is a frequently assessed feature of roden
221 of the anti-phase pattern during the second postnatal week is accompanied by increased diurnal wakef
222 te that Fth synthesis during the first three postnatal weeks is important for an appropriate oligoden
223 d at higher levels in the embryo and earlier postnatal weeks, it is also expressed in the adult rat b
224 el during three postnatal periods: the 4(th) postnatal week (juvenile ELE, P21-27), 6(th) postnatal w
226 V2 connectivity were in place as early as 2 postnatal weeks, labeled cells in V1 and V2 became more
227 that mediate retinal waves during the first postnatal week leads to the generation of "recovered" wa
228 tically enhance sensory inputs in the second postnatal week led to a significant increase in spine de
229 x accessory proteins at the end of the third postnatal week likely "turns on" the hippocampus by incr
232 This asymmetry emerges during the second postnatal week of development, but its basis remains unk
238 op spontaneous seizures during the first six postnatal weeks of life and brain slices show neuronal h
240 unctional histamine receptors from the first postnatal week onwards, with histamine having diverse ef
241 stamine receptors in striatum from the first postnatal week onwards, with pronounced developmental in
244 average across genotypes early in the first postnatal week [postnatal day 3 (P3) to P4] and, interes
245 rly deprived for 2 d at the end of the third postnatal week (pre-CP), whereas potentiation is induced
246 in (TARP) expression at the end of the third postnatal week provide a molecular explanation for the i
248 SGCs were of equal strength during the first postnatal week, regardless of whether the SAC was locate
249 m, primarily the cerebellum, the first three postnatal weeks represent a period of significant sensit
250 ed from newborn and adult mice (2nd and 12th postnatal weeks, respectively), were seeded at low (5 ce
252 tion shape spike-timing, VGNs from the first postnatal week respond to synaptic-noise-like current in
254 ked ventral root potentials until the second postnatal week, revealing a late role for spindle-derive
255 spherules begin to retract during the second postnatal week, rod bipolar cells initially show no sign
257 igodendrocytes during the first or the third postnatal week significantly reduces oligodendrocyte iro
259 d no defects in the retina before the second postnatal week, suggesting that miRNAs are not required
260 lover excitation persisted beyond the second postnatal week, suggesting that this mechanism may play
261 already established by the first and second postnatal weeks, suggesting guidance through intrinsic d
264 se proteins were KO in vivo during the first postnatal week, the sciatic nerve of all 3 conditional K
266 ation was present throughout the first three postnatal weeks, the size of input maps was developmenta
267 ittermates at the end of the first and third postnatal weeks, the Ts65Dn animals showed significantly
268 subplate neurons, whereas, during the second postnatal week, these AMPARs were highly expressed on co
269 icited in some NG2(+) cells during the first postnatal week, they were not capable of generating acti
270 dense time course sampling between 4 and 20 postnatal weeks to characterize early transcriptomic, mo
271 of mouse auditory cortex during the first 2 postnatal weeks to study the spatial origin of silent sy
272 vocal sequences, we found that in the first postnatal week, twins had more similar vocal sequences t
273 , Rem2 mRNA and protein expression peaked at postnatal week two, which corresponds to the period of r
274 curring for both D1 and D2 SPNs in the first postnatal weeks using in vitro whole-cell patch-clamp el
275 th acutely and longer-term, during the first postnatal weeks, using patch-clamp and field recordings
277 Daily administration of OT in the first postnatal week was sufficient to prevent deficits in soc
278 ty, which is normally lost during the second postnatal week, was maintained and synaptic competition
282 t in CHL1 (lacking CHL1 only after the third postnatal week) were tested relative to littermate contr
283 B-containing NMDARs prevail until the second postnatal week when GluN2A subunits are progressively ad
284 in the rodent hippocampus during the second postnatal week when most synapses become established and
285 in Norway rats around the end of the second postnatal week when nocturnal wakefulness and the in-pha
286 and proliferation in TBCs during the first 3 postnatal weeks, when the number of TBCs decreases.
287 cesses that occur primarily during the first postnatal week, whereas neurogenesis and migration showe
288 within a narrow range during the first three postnatal weeks, whereas glycinergic ones exhibited age-
289 edforward inhibition at the end of the first postnatal week, which has profound effects on circuit fu
291 -deficient horizontal cells during the first postnatal weeks, which dropped off abruptly by P30.
292 ication of zinc sulfate during the first two postnatal weeks, which interferes with their ability to
293 Bergmann glia are generated up to first the postnatal weeks, which was proposed to be neurogenic.
294 quantal amplitudes increase during the first postnatal week while the prevalence of silent synapses d
297 ty begins to decline by the end of the first postnatal week, with approximately 25% of SGNs ultimatel
298 owed a gentle plateau throughout the first 3 postnatal weeks, with only a slight decline of BDNF expr
299 and gradually decreased over the first three postnatal weeks within the hippocampus, amygdala, striat
300 discrete cell clusters emerge over the first postnatal week, yielding an identifiable modular network