Increased Oxidative Metabolism and Neurotransmitter Cycling in the Brain of Mice Lacking the Thyroid Hormone Transporter Slc16a2 (Mct8)

Rodrigues, Tiago B.; Ceballos, Ainhoa; Grijota-Martínez, Carmen; Núñez, Bárbara; Refetoff, Samuel; Cerdán, Sebastián; Morte, Beatriz; Bernal, Juan

doi:10.1371/journal.pone.0074621

Cited by 18 publications

(14 citation statements)

References 49 publications

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“…In order to elucidate the pathophysiological mechanisms of AHDS, an MCT8 knockout (KO) mouse model was generated. These KO mice replicate the endocrine and metabolic abnormalities found in human patients [9] – [12] . However, they did not display any neurological or behavioral phenotypes.…”

Section: Introductionsupporting

confidence: 64%

Altered Behavioral Performance and Live Imaging of Circuit-Specific Neural Deficiencies in a Zebrafish Model for Psychomotor Retardation

et al. 2014

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The mechanisms and treatment of psychomotor retardation, which includes motor and cognitive impairment, are indefinite. The Allan-Herndon-Dudley syndrome (AHDS) is an X-linked psychomotor retardation characterized by delayed development, severe intellectual disability, muscle hypotonia, and spastic paraplegia, in combination with disturbed thyroid hormone (TH) parameters. AHDS has been associated with mutations in the monocarboxylate transporter 8 (mct8/slc16a2) gene, which is a TH transporter. In order to determine the pathophysiological mechanisms of AHDS, MCT8 knockout mice were intensively studied. Although these mice faithfully replicated the abnormal serum TH levels, they failed to exhibit the neurological and behavioral symptoms of AHDS patients. Here, we generated an mct8 mutant (mct8−/−) zebrafish using zinc-finger nuclease (ZFN)-mediated targeted gene editing system. The elimination of MCT8 decreased the expression levels of TH receptors; however, it did not affect the expression of other TH-related genes. Similar to human patients, mct8−/− larvae exhibited neurological and behavioral deficiencies. High-throughput behavioral assays demonstrated that mct8−/− larvae exhibited reduced locomotor activity, altered response to external light and dark transitions and an increase in sleep time. These deficiencies in behavioral performance were associated with altered expression of myelin-related genes and neuron-specific deficiencies in circuit formation. Time-lapse imaging of single-axon arbors and synapses in live mct8−/− larvae revealed a reduction in filopodia dynamics and axon branching in sensory neurons and decreased synaptic density in motor neurons. These phenotypes enable assessment of the therapeutic potential of three TH analogs that can enter the cells in the absence of MCT8. The TH analogs restored the myelin and axon outgrowth deficiencies in mct8−/− larvae. These findings suggest a mechanism by which MCT8 regulates neural circuit assembly, ultimately mediating sensory and motor control of behavioral performance. We also propose that the administration of TH analogs early during embryo development can specifically reduce neurological damage in AHDS patients.

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Section: Introductionsupporting

confidence: 64%

Altered Behavioral Performance and Live Imaging of Circuit-Specific Neural Deficiencies in a Zebrafish Model for Psychomotor Retardation

et al. 2014

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“…The clinically relevant dose of T4 for the neonatal mouse is unknown, however the dose used in this study maintains the normal physiological levels of T4 when administered to adult hypothyroid mice (Rodrigues et al, 2013). Euthyroid treatment is critical as overexposure to TH may have negative effects on the brain (Nicholson and Altman, 1972), and TH repression of TSH can cause hypothyroidism upon completion of therapy (La Gamma et al, 2009).…”

Section: Discussionmentioning

confidence: 99%

Failure of thyroid hormone treatment to prevent inflammation-induced white matter injury in the immature brain

Schang

Steenwinckel

Chevenne

et al. 2014

Brain, Behavior, and Immunity

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“…In order to study the mechanism underlying AHDS, an Mct8 knockout ( Mct8 -KO) mouse model was established. Similar to individuals with AHDS, the Mct8 -KO mice showed altered TH levels in the serum; however, neurological and behavioral phenotypes were not apparent (Di Cosmo et al, 2013; Dumitrescu et al, 2006; Rodrigues et al, 2013; Trajkovic et al, 2007). This might be explained by a compensation mechanism in mice in which the organic anion transporting polypeptide 1C1 ( Oatp1c1 ), a T4-selective transporter, is predominantly expressed in the BBB (Ito et al, 2011; Mayerl et al, 2012; Roberts et al, 2008).…”

Section: Introductionmentioning

confidence: 87%

Pharmacological treatment and BBB-targeted genetic therapy for MCT8-dependent hypomyelination in zebrafish

Zada

Tovin

Lerer-Goldshtein

et al. 2016

Disease Models &Amp; Mechanisms

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Hypomyelination is a key symptom of Allan-Herndon-Dudley syndrome (AHDS), a psychomotor retardation associated with mutations in the thyroid-hormone (TH) transporter MCT8 (monocarboxylate transporter 8). AHDS is characterized by severe intellectual deficiency, neuromuscular impairment and brain hypothyroidism. In order to understand the mechanism for TH-dependent hypomyelination, we developed an mct8 mutant (mct8−/−) zebrafish model. The quantification of genetic markers for oligodendrocyte progenitor cells (OPCs) and mature oligodendrocytes revealed reduced differentiation of OPCs into oligodendrocytes in mct8−/− larvae and adults. Live imaging of single glial cells showed that the number of oligodendrocytes and the length of their extensions are reduced, and the number of peripheral Schwann cells is increased, in mct8−/− larvae compared with wild type. Pharmacological analysis showed that TH analogs and clemastine partially rescued the hypomyelination in the CNS of mct8−/− larvae. Intriguingly, triiodothyronine (T3) treatment rescued hypomyelination in mct8−/− embryos before the maturation of the blood–brain barrier (BBB), but did not affect hypomyelination in older larvae. Thus, we expressed Mct8-tagRFP in the endothelial cells of the vascular system and showed that even relatively weak mosaic expression completely rescued hypomyelination in mct8−/− larvae. These results suggest potential pharmacological treatments and BBB-targeted gene therapy that can enhance myelination in AHDS and possibly in other TH-dependent brain disorders.

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Increased Oxidative Metabolism and Neurotransmitter Cycling in the Brain of Mice Lacking the Thyroid Hormone Transporter Slc16a2 (Mct8)

Cited by 18 publications

References 49 publications

Altered Behavioral Performance and Live Imaging of Circuit-Specific Neural Deficiencies in a Zebrafish Model for Psychomotor Retardation

Altered Behavioral Performance and Live Imaging of Circuit-Specific Neural Deficiencies in a Zebrafish Model for Psychomotor Retardation

Failure of thyroid hormone treatment to prevent inflammation-induced white matter injury in the immature brain

Pharmacological treatment and BBB-targeted genetic therapy for MCT8-dependent hypomyelination in zebrafish

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