Adaptation Insights from Comparative Transcriptome Analysis of Two Opisthopappus Species in the Taihang Mountains

Abstract Opisthopappus is a major wild source of Asteraceae with good cold and drought resistance. Two species of this genus (Opisthopappus taihangensis and Opisthopappus longilobus) have been employed as model systems to address the evolutionary history of perennial herb biomes in the Taihang Mountains of China. However, further studies on the adaptive divergence processes of these two species are currently impeded by the lack of genomic resources. To elucidate the molecular mechanisms involved, a comparative analysis of these two species was conducted. Among the identified transcription factors, the bHLH members were most prevalent, which exhibited significantly different expression levels in the terpenoid metabolic pathway. O. longilobus revealed a higher expression than did O. taihangensis in terms of terpenes biosynthesis and metabolism, particularly regarding monoterpenoids and diterpenoids. Analyses of the positive selection genes (PSGs) identified from O. taihangensis and O. longilobus, 1203 genes were found that related to adaptative divergence, which were under rapid evolution and/or have signs of positive selection. Different PSG expressions occurred primarily in the mitochondrial electron transport, starch degradation, secondary metabolism, as well as nucleotide synthesis and S-metabolism pathway processes. Two PSGs were obviously differentially expressed in terpenes biosynthesis that might result in the fragrances divergence between O. longilobus and O. taihangensis, which would provide insights as to how the two species adapted to different environments, characterized by sub-humid warm temperate and temperate continental monsoon climates. The comparative analysis for these two species of Opisthopappus not only revealed how the divergence occurred from molecular perspective, but also provided novel insights into how differential adaptations occurred in Taihang Mountains.

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Regulation of microRNAs in Inflammation-Associated Colorectal Cancer: A Mechanistic Approach

Endocrine Metabolic & Immune Disorders - Drug Targets ◽

10.2174/1871530320666200917112802 ◽

2020 ◽

Vol 20 ◽

Author(s):

Sridhar Muthusami ◽

Ilangovan Ramachandran ◽

Sneha Krishnamoorthy ◽

Yuvaraj Sambandam ◽

Satish Ramalingam ◽

...

Keyword(s):

Colorectal Cancer ◽

Molecular Mechanisms ◽

Colorectal Carcinogenesis ◽

Model Systems ◽

Necrosis Factor Alpha ◽

Multi Stage ◽

Mechanistic Approach ◽

Tnf Α ◽

Factor Alpha

: The development of colorectal cancer (CRC) is a multi-stage process. The inflammation of the colon as in inflammatory bowel disease (IBD) such as ulcerative colitis (UC) or Crohn’s disease (CD) is often regarded as the initial trigger for the development of CRC. Many cytokines such as tumor necrosis factor alpha (TNF-α) and several interleukins (ILs) are known to exert proinflammatory actions, and inflammation initiates or promotes tumorigenesis of various cancers, including CRC through differential regulation of microRNAs (miRNAs/miRs). miRNAs can be oncogenic miRNAs (oncomiRs) or anti-oncomiRs/tumor suppressor miRNAs, and they play key roles during colorectal carcinogenesis. However, the functions and molecular mechanisms of regulation of miRNAs involved in inflammation-associated CRC are still anecdotal and largely unknown. Consolidating the published results and offering perspective solutions to circumvent CRC, the current review is focused on the role of miRNAs and their regulation in the development of CRC. We have also discussed the model systems adapted by researchers to delineate the role of miRNAs in inflammation-associated CRC.

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The TGFβ Family in Human Placental Development at the Fetal-Maternal Interface

Biomolecules ◽

10.3390/biom10030453 ◽

2020 ◽

Vol 10 (3) ◽

pp. 453

Author(s):

Susana M. Chuva de Sousa Lopes ◽

Marta S. Alexdottir ◽

Gudrun Valdimarsdottir

Keyword(s):

Stem Cell ◽

Transforming Growth Factor Beta ◽

Molecular Mechanisms ◽

Transforming Growth Factor ◽

Cell Model ◽

Embryonic Stem ◽

Model Systems ◽

Special Focus ◽

Placental Development

Emerging data suggest that a trophoblast stem cell (TSC) population exists in the early human placenta. However, in vitro stem cell culture models are still in development and it remains under debate how well they reflect primary trophoblast (TB) cells. The absence of robust protocols to generate TSCs from humans has resulted in limited knowledge of the molecular mechanisms that regulate human placental development and TB lineage specification when compared to other human embryonic stem cells (hESCs). As placentation in mouse and human differ considerably, it is only with the development of human-based disease models using TSCs that we will be able to understand the various diseases caused by abnormal placentation in humans, such as preeclampsia. In this review, we summarize the knowledge on normal human placental development, the placental disease preeclampsia, and current stem cell model systems used to mimic TB differentiation. A special focus is given to the transforming growth factor-beta (TGFβ) family as it has been shown that the TGFβ family has an important role in human placental development and disease.

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Unveiling the Dynamics of KRAS4b on Lipid Model Membranes

The Journal of Membrane Biology ◽

10.1007/s00232-021-00176-z ◽

2021 ◽

Author(s):

Cesar A. López ◽

Animesh Agarwal ◽

Que N. Van ◽

Andrew G. Stephen ◽

S. Gnanakaran

Keyword(s):

Molecular Mechanisms ◽

Hypervariable Region ◽

Small Gtpase ◽

Model Systems ◽

Coarse Grained ◽

Regulatory Function ◽

Limited Information ◽

Long Time ◽

Cell Growth And Differentiation ◽

State Models

AbstractSmall GTPase proteins are ubiquitous and responsible for regulating several processes related to cell growth and differentiation. Mutations that stabilize their active state can lead to uncontrolled cell proliferation and cancer. Although these proteins are well characterized at the cellular scale, the molecular mechanisms governing their functions are still poorly understood. In addition, there is limited information about the regulatory function of the cell membrane which supports their activity. Thus, we have studied the dynamics and conformations of the farnesylated KRAS4b in various membrane model systems, ranging from binary fluid mixtures to heterogeneous raft mimics. Our approach combines long time-scale coarse-grained (CG) simulations and Markov state models to dissect the membrane-supported dynamics of KRAS4b. Our simulations reveal that protein dynamics is mainly modulated by the presence of anionic lipids and to some extent by the nucleotide state (activation) of the protein. In addition, our results suggest that both the farnesyl and the polybasic hypervariable region (HVR) are responsible for its preferential partitioning within the liquid-disordered (Ld) domains in membranes, potentially enhancing the formation of membrane-driven signaling platforms. Graphic Abstract

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Comparative Analysis of Latex Transcriptome Reveals Putative Molecular Mechanisms Underlying Super Productivity of Hevea brasiliensis

PLoS ONE ◽

10.1371/journal.pone.0075307 ◽

2013 ◽

Vol 8 (9) ◽

pp. e75307 ◽

Cited By ~ 21

Author(s):

Chaorong Tang ◽

Xiaohu Xiao ◽

Heping Li ◽

Yujie Fan ◽

Jianghua Yang ◽

...

Keyword(s):

Comparative Analysis ◽

Hevea Brasiliensis ◽

Molecular Mechanisms

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TMOD-02. GENERATION OF A NOVEL MOUSE MODEL FOR BRAIN TUMORS OF THE DNA METHYLATION CLASS “GBM MYCN”

Neuro-Oncology ◽

10.1093/neuonc/noab196.864 ◽

2021 ◽

Vol 23 (Supplement_6) ◽

pp. vi215-vi216

Author(s):

Melanie Schoof ◽

Carolin Göbel ◽

Dörthe Holdhof ◽

Sina Al-Kershi ◽

Ulrich Schüller

Keyword(s):

Dna Methylation ◽

Brain Tumors ◽

Molecular Mechanisms ◽

Treatment Options ◽

Tumor Development ◽

Model Systems ◽

Preclinical Research ◽

Human Gbm

Abstract DNA methylation based classification of brain tumors has revealed a high heterogeneity between tumors and led to the description of multiple distinct subclasses. The increasing subdivision of tumors can help to understand molecular mechanisms of tumor development and to improve therapy if appropriate model systems for preclinical research are available. Multiple recent publications have described a subgroup of pediatric glioblastoma which is clearly separable from other pediatric and adult glioblastoma in its DNA methylation profile (GBM MYCN). Many cases in this group are driven by MYCN amplifications and harbor TP53 mutations. These tumors almost exclusively occur in children and were further described as highly aggressive with a median overall survival of only 14 months. In order to further investigate the biology and treatment options of these tumors, we generated hGFAP-cre::TP53 Fl/Fl ::lsl-MYCN mice. These mice carry a loss of TP53 and show aberrant MYCN expression in neural precursors of the central nervous system. The animals develop large forebrain tumors within the first 80 days of life with 100 % penetrance. These tumors resemble human GBM MYCN tumors histologically and are sensitive to AURKA and ATR inhibitors in vitro. We believe that further characterization of the model and in vivo treatment studies will pave the way to improve treatment of patients with these highly aggressive tumors.

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Creating model systems to study molecular mechanisms of C5 convertase-induced Membrane Attack Complex assembly

Molecular Immunology ◽

10.1016/j.molimm.2017.06.124 ◽

2017 ◽

Vol 89 ◽

pp. 160

Author(s):

D.J. Doorduijn ◽

R.D. Gorham ◽

L. van Bloois ◽

E. Mastrobattista ◽

S.H.M. Rooijakkers

Keyword(s):

Molecular Mechanisms ◽

Membrane Attack Complex ◽

Model Systems ◽

Complex Assembly ◽

Induced Membrane

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Rapid, ultra-local adaptation facilitated by phenotypic plasticity

10.1101/598292 ◽

2019 ◽

Author(s):

Syuan-Jyun Sun ◽

Andrew M. Catherall ◽

Sonia Pascoal ◽

Benjamin J. M. Jarrett ◽

Sara E. Miller ◽

...

Keyword(s):

Gene Flow ◽

Rapid Evolution ◽

Reaction Norm ◽

Ancestral Population ◽

Adaptive Divergence ◽

Wild Populations ◽

Rapid Adaptation ◽

Burying Beetles ◽

Genetic Accommodation ◽

Nicrophorus Vespilloides

AbstractModels of ‘plasticity-first’ evolution are attractive because they explain the rapid evolution of new complex adaptations. Nevertheless, it is unclear whether plasticity can still facilitate rapid evolution when diverging populations are connected by gene flow. Here we show how plasticity has generated adaptive divergence in fecundity in wild populations of burying beetlesNicrophorus vespilloides, which are still connected by gene flow, which occupy distinct Cambridgeshire woodlands that are just 2.5km apart and which diverged from a common ancestral population c. 1000-4000 years ago. We show that adaptive divergence is duetothe coupling of an evolved increase in the elevation of the reaction norm linking clutch size to carrion size (i.e. genetic accommodation) with plastic secondary elimination of surplus offspring. Working in combination, these two processes have facilitated rapid adaptation to fine-scale environmental differences, despite ongoing gene flow.

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Discovering the drivers of clonal hematopoiesis

10.1101/2020.10.22.350140 ◽

2020 ◽

Cited By ~ 1

Author(s):

Oriol Pich ◽

Iker Reyes-Salazar ◽

Abel Gonzalez-Perez ◽

Nuria Lopez-Bigas

Keyword(s):

Positive Selection ◽

Molecular Mechanisms ◽

Somatic Mutations ◽

Cancer Genomics ◽

Variant Calling ◽

Selective Advantage ◽

Cancer Genes ◽

Driver Genes ◽

Hematopoietic Stem ◽

Clonal Hematopoiesis

AbstractMutations in genes that confer a selective advantage to hematopoietic stem cells (HSCs) in certain conditions drive clonal hematopoiesis (CH). While some CH drivers have been identified experimentally or through epidemiological studies, the compendium of all genes able to drive CH upon mutations in HSCs is far from complete. We propose that identifying signals of positive selection in blood somatic mutations may be an effective way to identify CH driver genes, similarly as done to identify cancer genes. Using a reverse somatic variant calling approach, we repurposed whole-genome and whole-exome blood/tumor paired samples of more than 12,000 donors from two large cancer genomics cohorts to identify blood somatic mutations. The application of IntOGen, a robust driver discovery pipeline, to blood somatic mutations across both cohorts, and more than 24,000 targeted sequenced samples yielded a list of close to 70 genes with signals of positive selection in CH, available at http://www.intogen.org/ch. This approach recovers all known CH genes, and discovers novel candidates. Generating this compendium is an essential step to understand the molecular mechanisms of CH and to accurately detect individuals with CH to ascertain their risk to develop related diseases.

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Genomic evidence of adaptive evolution in the reptilian SOCS gene family

PeerJ ◽

10.7717/peerj.11677 ◽

2021 ◽

Vol 9 ◽

pp. e11677

Author(s):

Tian Xia ◽

Lei Zhang ◽

Guolei Sun ◽

Xiufeng Yang ◽

Honghai Zhang

Keyword(s):

Negative Selection ◽

Molecular Mechanisms ◽

Evolutionary Dynamics ◽

Theoretical Foundation ◽

Selective Pressure ◽

Rapid Evolution ◽

Cytokine Signaling ◽

Signal Pathways ◽

Branch Model ◽

Comprehensive Study

The suppressor of the cytokine signaling (SOCS) family of proteins play an essential role in inhibiting cytokine receptor signaling by regulating immune signal pathways. Although SOCS gene functions have been examined extensively, no comprehensive study has been performed on this gene family’s molecular evolution in reptiles. In this study, we identified eight canonical SOCS genes using recently-published reptilian genomes. We used phylogenetic analysis to determine that the SOCS genes had highly conserved evolutionary dynamics that we classified into two types. We identified positive SOCS4 selection signals in whole reptile lineages and SOCS2 selection signals in the crocodilian lineage. Selective pressure analyses using the branch model and Z-test revealed that these genes were under different negative selection pressures compared to reptile lineages. We also concluded that the nature of selection pressure varies across different reptile lineages on SOCS3, and the crocodilian lineage has experienced rapid evolution. Our results may provide a theoretical foundation for further analyses of reptilian SOCS genes’ functional and molecular mechanisms, as well as their roles in reptile growth and development.

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Protein Kinase C Signaling Mediates a Program of Cell Cycle Withdrawal in the Intestinal Epithelium

The Journal of Cell Biology ◽

10.1083/jcb.151.4.763 ◽

2000 ◽

Vol 151 (4) ◽

pp. 763-778 ◽

Cited By ~ 81

Author(s):

Mark R. Frey ◽

Jennifer A. Clark ◽

Olga Leontieva ◽

Joshua M. Uronis ◽

Adrian R. Black ◽

...

Keyword(s):

Cell Cycle ◽

Protein Kinase C ◽

Protein Kinase ◽

Intestinal Epithelium ◽

Molecular Mechanisms ◽

Model Systems ◽

Intestinal Epithelial ◽

Kinase C

Members of the protein kinase C (PKC) family of signal transduction molecules have been widely implicated in regulation of cell growth and differentiation, although the underlying molecular mechanisms involved remain poorly defined. Using combined in vitro and in vivo intestinal epithelial model systems, we demonstrate that PKC signaling can trigger a coordinated program of molecular events leading to cell cycle withdrawal into G0. PKC activation in the IEC-18 intestinal crypt cell line resulted in rapid downregulation of D-type cyclins and differential induction of p21waf1/cip1 and p27kip1, thus targeting all of the major G1/S cyclin-dependent kinase complexes. These events were associated with coordinated alterations in expression and phosphorylation of the pocket proteins p107, pRb, and p130 that drive cells to exit the cell cycle into G0 as indicated by concomitant downregulation of the DNA licensing factor cdc6. Manipulation of PKC isozyme levels in IEC-18 cells demonstrated that PKCα alone can trigger hallmark events of cell cycle withdrawal in intestinal epithelial cells. Notably, analysis of the developmental control of cell cycle regulatory molecules along the crypt–villus axis revealed that PKCα activation is appropriately positioned within intestinal crypts to trigger this program of cell cycle exit–specific events in situ. Together, these data point to PKCα as a key regulator of cell cycle withdrawal in the intestinal epithelium.

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