Time is of the essence: the molecular mechanisms of primary microcephaly

Phan, Thao P; Holland, Andrew J.

doi:10.1101/gad.348866.121

Cited by 58 publications

(60 citation statements)

References 331 publications

(312 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Despite the diverse genetic causes, microcephaly phenotypes often converge to trigger p53 activation and apoptosis in dividing RGPs and/or nascent neurons. In such cases, genetic deletion of Trp53 rescues the microcephaly phenotype ( 41 – 44 ). We noted the presence of p53-related GO terms in several modules of the STRING network (data table S1).…”

Section: Resultsmentioning

confidence: 99%

Tissue-wide genetic and cellular landscape shapes the execution of sequential PRC2 functions in neural stem cell lineage progression

et al. 2022

View full text Add to dashboard Cite

The generation of a correctly sized cerebral cortex with all-embracing neuronal and glial cell–type diversity critically depends on faithful radial glial progenitor (RGP) cell proliferation/differentiation programs. Temporal RGP lineage progression is regulated by Polycomb repressive complex 2 (PRC2), and loss of PRC2 activity results in severe neurogenesis defects and microcephaly. How PRC2-dependent gene expression instructs RGP lineage progression is unknown. Here, we use mosaic analysis with double markers (MADM)–based single-cell technology and demonstrate that PRC2 is not cell-autonomously required in neurogenic RGPs but rather acts at the global tissue-wide level. Conversely, cortical astrocyte production and maturation is cell-autonomously controlled by PRC2-dependent transcriptional regulation. We thus reveal highly distinct and sequential PRC2 functions in RGP lineage progression that are dependent on complex interplays between intrinsic and tissue-wide properties. In a broader context, our results imply a critical role for the genetic and cellular niche environment in neural stem cell behavior.

show abstract

Section: Resultsmentioning

confidence: 99%

Tissue-wide genetic and cellular landscape shapes the execution of sequential PRC2 functions in neural stem cell lineage progression

et al. 2022

View full text Add to dashboard Cite

show abstract

“…By consensus, MCPH is thought to be a consequence of neural progenitor depletion/premature differentiation (Jayaraman et al, 2018; Phan & Holland, 2021). For instance, in MCPH3 (caused by mutations in CDK5RAP2) (Lancaster et al, 2013), MCPH5 (ASPM) (R. Li et al, 2017), and MCPH6 (CENPJ) (Bond et al, 2005), neural progenitors at the Ventricular Zone (VZ)/Sub-Ventricular Zone (SVZ) lose their broad proliferative capacity impacting final brain architecture and size (Gabriel et al, 2020; Phan & Holland, 2021). For this reason, we sought to determine whether the WDR62 mutation might impact NES cell features.…”

Section: Resultsmentioning

confidence: 99%

“…Mutations in genes involved in the regulation of mitotic progression in neural progenitor cells (NPCs) have been identified in several types of MCPH (Phan & Holland, 2021; Thornton & Woods, 2009), a genetically heterogeneous disorder characterized by occipito-frontal circumference 3-4 standard deviations below the mean of ethnically-, age-, and sex-matched controls (Woods & Parker, 2013). Intriguingly, many of the genes associated with MCPH encode centrosomal or pericentriolar proteins, while others participate in mitotic spindle organization and mitotic progression (Jayaraman et al, 2018; Phan & Holland, 2021).…”

Section: Introductionmentioning

confidence: 99%

Microcephaly-associated WDR62 mutations hamper Golgi apparatus-to-spindle pole shuttling in human neural progenitors

Dell’Amico

Salavarria

Takeo

et al. 2022

Preprint

View full text Add to dashboard Cite

WDR62 is a spindle pole-associated scaffold protein with pleiotropic functions during corticogenesis. Recessive mutations in WDR62 are associated with structural brain abnormalities and account for the second most common cause of autosomal recessive primary microcephaly (MCPH), indicating WDR62 as a critical hub for human brain development. Here, we investigated a C-terminal truncating mutation (D955AfsX112) in WDR62 using induced pluripotent stem cells (iPSCs) obtained from a patient with MCPH2. We generated neuroepithelial stem (NES) cells and cerebro-cortical progenitors and neurons from patient-derived and isogenic retro-mutated iPSC lines. We found that WDR62 dysfunction resulted in impaired cell cycle progression and alterations of the neurogenic trajectories of iPSC neuroderivatives. Moreover, we report WDR62 localization at the Golgi apparatus during interphase, both in human neural progenitors in vitro and in human fetal brain tissue. WDR62 shuttling from the Golgi apparatus to spindle poles is dynamic and microtubule-dependent. Impairment of WDR62 function and localization results in severe neurodevelopmental abnormalities, thus delineating new mechanisms in MCPH etiology.

show abstract

“…Human diseases characterized by chromosomal instability are typically associated to mutations in genes related to cell division. Mutations in genes associated with centrosome and microtubule dynamics, chromosome morphology, and kinetochore functions affect the majority of patients with primary microcephaly ( 3 ), and alteration of different cohesin subunits and associated regulators results in a variety of pathologies known as cohesinopathies ( 4 ). Aneuploidy, however, is only occasionally observed in these pathologies ( 4 ).…”

Section: Introductionmentioning

confidence: 99%

Biallelic germline mutations in MAD1L1 induce a syndrome of aneuploidy with high tumor susceptibility

et al. 2022

View full text Add to dashboard Cite

Germline mutations leading to aneuploidy are rare, and their tumor-promoting properties are mostly unknown at the molecular level. We report here novel germline biallelic mutations in MAD1L1 , encoding the spindle assembly checkpoint (SAC) protein MAD1, in a 36-year-old female with a dozen of neoplasias. Functional studies demonstrated lack of full-length protein and deficient SAC response, resulting in ~30 to 40% of aneuploid blood cells. Single-cell RNA analysis identified mitochondrial stress accompanied by systemic inflammation with enhanced interferon and NFκB signaling both in aneuploid and euploid cells, suggesting a non–cell autonomous response. MAD1L1 mutations resulted in specific clonal expansions of γδ T cells with chromosome 18 gains and enhanced cytotoxic profile as well as intermediate B cells with chromosome 12 gains and transcriptomic signatures characteristic of leukemia cells. These data point to MAD1L1 mutations as the cause of a new variant of mosaic variegated aneuploidy with systemic inflammation and unprecedented tumor susceptibility.

show abstract

Time is of the essence: the molecular mechanisms of primary microcephaly

Cited by 58 publications

References 331 publications

Tissue-wide genetic and cellular landscape shapes the execution of sequential PRC2 functions in neural stem cell lineage progression

Tissue-wide genetic and cellular landscape shapes the execution of sequential PRC2 functions in neural stem cell lineage progression

Microcephaly-associated WDR62 mutations hamper Golgi apparatus-to-spindle pole shuttling in human neural progenitors

Biallelic germline mutations in MAD1L1 induce a syndrome of aneuploidy with high tumor susceptibility

Contact Info

Product

Resources

About