Publications by authors named "Matko Gluncic"

Motivation: Tandem monomeric units, integral components of eukaryotic genomes, form higher-order repeat (HOR) structures that play crucial roles in maintaining chromosome integrity and regulating gene expression and protein abundance. Given their significant influence on processes such as evolution, chromosome segregation, and disease, developing a sensitive and automated tool for identifying HORs across diverse genomic sequences is essential.

Results: In this study, we applied the GRMhor (Global Repeat Map hor) algorithm to analyse the centromeric region of chromosome 20 in three individual human genomes, as well as in the centromeric regions of three higher primates.

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From the recent genome assembly NHGRI_mPonAbe1-v2.0_NCBI (GCF_028885655.2) of orangutan chromosome 13, we computed the precise alpha satellite higher-order repeat (HOR) structure using the novel high-precision GRM2023 algorithm with Global Repeat Map (GRM) and Monomer Distance (MD) diagrams.

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Aim: To precisely identify and analyze alpha-satellite higher-order repeats (HORs) in T2T-CHM13 assembly of human chromosome 3.

Methods: From the recently sequenced complete T2T-CHM13 assembly of human chromosome 3, the precise alpha satellite HOR structure was computed by using the novel high-precision GRM2023 algorithm with global repeat map (GRM) and monomer distance (MD) diagrams.

Results: The major alpha satellite HOR array in chromosome 3 revealed a novel cascading HOR, housing 17mer HOR copies with subfragments of periods 15 and 2.

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Unraveling the intricate centromere structure of human chromosomes holds profound implications, illuminating fundamental genetic mechanisms and potentially advancing our comprehension of genetic disorders and therapeutic interventions. This study rigorously identified and structurally analyzed alpha satellite higher-order repeats (HORs) within the centromere of human chromosome 15 in the complete T2T-CHM13 assembly using the high-precision GRM2023 algorithm. The most extensive alpha satellite HOR array in chromosome 15 reveals a novel cascading HOR, housing 429 15mer HOR copies, containing 4-, 7- and 11-monomer subfragments.

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Article Synopsis
  • The NBPF repeats, specifically the 3mer HORs, are unique to humans and are believed to play a role in cognitive abilities, showing a significant increase from chimpanzees to modern humans.
  • Research on the Neanderthal genome revealed that while it also has NBPF 3mer HOR arrays, their structure and number differ from those found in modern humans.
  • The study identified two new types of NBPF 3mer HOR arrays in the complete human genome, which may correspond to novel genes, suggesting that further exploration of the Neanderthal genome could enhance our understanding of human evolution.
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In this article, we show that mono/oligonucleotide quadruplets, as basic structures of DNA, along with our classification of trinucleotides, disclose an organization of genomes based on purine-pyrimidine symmetry. Moreover, the structure and stability of DNA are influenced by the Watson-Crick pairing and the natural law of DNA creation and conservation, according to which the same mono- or oligonucleotide insertion must be inserted simultaneously into both strands of DNA. Taken together, they lead to quadruplets with central mirror symmetry and bidirectional DNA strand orientation and are incorporated into Chargaff's second parity rule (CSPR).

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Previously it was found that the neuroblastoma breakpoint family () gene repeat units of ∼1.6 kb have an important role in human brain evolution and function. The higher order organization of these repeat units has been discovered by both methods, the higher order repeat (HOR)-searching method and the HLS searching method.

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Here we present three interesting novel human Higher-Order Repeats (HORs) discovered using the HOR-searching method with GRM algorithm: (a) The novel Neuroblastoma Breakpoint Family gene (NBPF) 3mer HOR, discovered applying GRM algorithm to human chromosome 1 (Paar et al., Mol Biol Evol 28:1877-1892, 2011). NBPF 3mer HOR is based on previously known ~1.

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The centromere is important for segregation of chromosomes during cell division in eukaryotes. Its destabilization results in chromosomal missegregation, aneuploidy, hallmarks of cancers and birth defects. In primate genomes centromeres contain tandem repeats of ~171 bp alpha satellite DNA, commonly organized into higher order repeats (HORs).

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Article Synopsis
  • * The study shows that kinesin-8 motors, specifically Klp5 and Klp6, are crucial for centering kinetochores and that these motors promote microtubule instability to facilitate movement.
  • * Researchers found that pulling forces drive kinetochore movement and that oscillations in movement can occur under various conditions, revealing the complex dynamics of microtubule behavior during chromosome alignment.
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Higher order repeats (HORs) containing tandems of primary and secondary repeat units (head-to-tail "tandem within tandem pattern"), referred to as regular HORs, are typical for primate alpha satellite DNAs and most pronounced in human genome. Regular HORs are known to be a result of recent evolutionary processes. In non-primate genomes mostly so called complex HORs have been found, without head to tail tandem of primary repeat units.

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Article Synopsis
  • * Research involving laser-cutting of k-fibres in HeLa and PtK1 cells indicates that these bridging fibres stabilize interkinetochore tension by connecting sister k-fibres and contain proteins like PRC1 and EB3, indicating they are formed by dynamic antiparallel microtubules.
  • * A theoretical model, supported by experimental results, reveals that the thickness of the bridging fibre impacts forces at both the pole and kineto
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For almost 50 years the conclusive explanation of Chargaff's second parity rule (CSPR), the equality of frequencies of nucleotides A=T and C=G or the equality of direct and reverse complement trinucleotides in the same DNA strand, has not been determined yet. Here, we relate CSPR to the interstrand mirror symmetry in 20 symbolic quadruplets of trinucleotides (direct, reverse complement, complement, and reverse) mapped to double-stranded genome. The symmetries of Q-box corresponding to quadruplets can be obtained as a consequence of Watson-Crick base pairing and CSPR together.

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Article Synopsis
  • In fission yeast, microtubules help center the nucleus by pushing against the cell's edge, but the specific role of kinesin-8 motors in this process was previously unclear.
  • Researchers created a physical model showing that kinesin-8 motors promote microtubule catastrophe, which aids in nuclear positioning.
  • Experimental results supported the model's predictions, demonstrating that with kinesin-8 motors, the nucleus centers better and predicting how quickly a displaced nucleus can return to the center.
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The origin and logic of genetic code are two of greatest mysteries of life sciences. Analyzing DNA sequences we showed that the start/stop trinucleotides have broader importance than just marking start and stop of exons in coding DNA. On this basis, here we introduced new classification of trinucleotides and showed that all A+T rich trinucleotides consisting of three different nucleotides arise from start-ATG, stop-TGA and stop-TAG using their complement, reverse complement and reverse transformations.

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The centromeres remain "the final frontier" in unexplored segments of genome landscape in primate genomes, characterized by 2-5 Mb arrays of evolutionary rapidly evolving alpha satellite (AS) higher order repeats (HORs). Alpha satellites as specific noncoding sequences may be also significant in light of regulatory role of noncoding sequences. Using the Global Repeat Map (GRM) algorithm we identify in NCBI assemblies of chromosome 5 the species-specific alpha satellite HORs: 13mer in human, 5mer in chimpanzee, 14mer in orangutan and 3mers in macaque.

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The main feature of global repeat map (GRM) algorithm (www.hazu.hr/grm/software/win/grm2012.

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Objective: The aim of this study was to identify the differences in the NRT measures, behavioral measures, and their relationship between the group of congenitally deaf children operated in the first years of life and the group of children operated in the school age.

Methods: The study included 40 congenitally deaf children with cochlear implants divided into two groups. Group 1 was composed of 20 children (mean age at operation 2.

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Article Synopsis
  • The study focuses on unique genomic patterns in humans that contribute to advanced cognitive abilities, particularly through the examination of noncoding DNA sequences that are present in humans but absent in chimpanzees.
  • Using a new computational approach, researchers identified higher order repeat structures (HORs) in human chromosome 1 that are associated with genes important for skin regeneration and brain function, which do not exist in chimpanzees.
  • The findings suggest that differences in these tandem repeat structures are more significant than differences in gene sequences between humans and chimpanzees, emphasizing the potential regulatory role of noncoding DNA in human evolution.
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Comparison of human and chimpanzee genomes has received much attention, because of paramount role for understanding evolutionary step distinguishing us from our closest living relative. In order to contribute to insight into Y chromosome evolutionary history, we study and compare tandems, higher order repeats (HORs), and regularly dispersed repeats in human and chimpanzee Y chromosome contigs, using robust Global Repeat Map algorithm. We find a new type of long-range acceleration, human-accelerated HOR regions.

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Article Synopsis
  • * The study focused on using DFT to analyze alphoid higher order repeats (HORs), revealing a distinct power spectrum with equidistant frequency patterns that indicate a two-level hierarchical organization.
  • * The findings demonstrate that DFT is effective for detecting higher order periodicities, showing a recognizable power spectrum characterized by both primary and secondary periodicity peaks, which remains consistent despite random variations in the DNA sequence.
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Key string algorithm (KSA) could be viewed as robust computational generalization of restriction enzyme method. KSA enables robust and effective identification and structural analyzes of any given genomic sequences, like in the case of NCBI assembly for human genome. We have developed a method, using total frequency distribution of all r-bp key strings in dependence on the fragment length l, to determine the exact size of all repeats within the given genomic sequence, both of monomeric and HOR type.

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Article Synopsis
  • Understanding how centromere DNA folds in condensed chromosomes is a key challenge in cell biology.
  • The study suggests new structural models showing how specific arrangements of alphoid higher order repeats (HORs) influence centromere folding.
  • These structures may help microtubules identify and interact with specific centromere configurations unique to each chromosome.
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Using our Key String Algorithm (KSA) to analyze Build 35.1 assembly we determined consensus alpha satellite higher-order repeats (HOR) and consensus distributions of CENP-B box and pJalpha motif in human chromosomes 1, 4, 5, 7, 8, 10, 11, 17, 19, and X. We determined new suprachromosomal family (SF) assignments: SF5 for 13mer (2211 bp), SF5 for 13mer (2214 bp), SF2 for 11mer (1869 bp), SF1 for 18mer (3058 bp), SF3 for 12mer (2047 bp), SF3 for 14mer (2379 bp), and SF5 for 17mer (2896 bp) in chromosomes 4, 5, 8, 10, 11, 17, and 19, respectively.

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Motivation: GenBank data are at present lacking alpha satellite higher-order repeat (HOR) annotation. Furthermore, exact HOR consensus lengths have not been reported so far. Given the fast growth of sequence databases in the centromeric region, it is of increasing interest to have efficient tools for computational identification and analysis of HORs from known sequences.

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