ABSTRACT
Superfamily Hominoidea, which consists of Hominidae (humans and great apes) and Hylobatidae (gibbons), is well-known for sharing human-like characteristics, however, the genomic origins of these shared unique phenotypes have mainly remained elusive. To decipher the underlying genomic basis of Hominoidea-restricted phenotypes, we identified and characterized Hominoidea-restricted highly conserved noncoding sequences (HCNSs) that are a class of potential regulatory elements which may be involved in evolution of lineage-specific phenotypes. We discovered 679 such HCNSs from human, chimpanzee, gorilla, orangutan and gibbon genomes. These HCNSs were demonstrated to be under purifying selection but with lineage-restricted characteristics different from old CNSs. A significant proportion of their ancestral sequences had accelerated rates of nucleotide substitutions, insertions and deletions during the evolution of common ancestor of Hominoidea, suggesting the intervention of positive Darwinian selection for creating those HCNSs. In contrary to enhancer elements and similar to silencer sequences, these Hominoidea-restricted HCNSs are located in close proximity of transcription start sites. Their target genes are enriched in the nervous system, development and transcription, and they tend to be remotely located from the nearest coding gene. Chip-seq signals and gene expression patterns suggest that Hominoidea-restricted HCNSs are likely to be functional regulatory elements by imposing silencing effects on their target genes in a tissue-restricted manner during fetal brain development. These HCNSs, emerged through adaptive evolution and conserved through purifying selection, represent a set of promising targets for future functional studies of the evolution of Hominoidea-restricted phenotypes.
Subject(s)
Brain/embryology , Gene Expression Regulation, Developmental , Hominidae/embryology , Hominidae/genetics , Animals , Base Sequence , Conserved Sequence , Epigenomics/methods , Evolution, Molecular , Gene Silencing , Gorilla gorilla/genetics , Humans , Hylobates/genetics , Pan troglodytes/genetics , Pongo pygmaeus/genetics , Regulatory Sequences, Nucleic AcidABSTRACT
Considerable variation exists in mandibular ramus form among primates, particularly great apes and humans. Recent analyses of adult ramal morphology have suggested that features on the ramus, especially the coronoid process and sigmoid notch, can be treated as phylogenetic characters that can be used to reconstruct relationships among great ape and fossil hominin taxa. Others have contended that ramal morphology is more influenced by function than phylogeny. In addition, it remains unclear how ontogeny of the ramus contributes to adult variation in great apes and humans. Specifically, it is unclear whether differences among adults appear early and are maintained throughout ontogeny, or if these differences appear, or are enhanced, during later development. To address these questions, the present study examined a broad ontogenetic sample of great apes and humans using two-dimensional geometric morphometric analysis. Variation within and among species was summarized using principal component and thin plate spline analyses, and Procrustes distances and discriminant function analyses were used to statistically compare species and age classes. Results suggest that morphological differences among species in ramal morphology appear early in ontogeny and persist into adulthood. Morphological differences among adults are particularly pronounced in the height and angulation of the coronoid process, the depth and anteroposterior length of the sigmoid notch, and the inclination of the ramus. In all taxa, the ascending ramus of the youngest specimens is more posteriorly inclined in relation to the occlusal plane, shifting to become more upright in adults. These results suggest that, although there are likely functional influences over the form of the coronoid process and ramus, the morphology of this region can be profitably used to differentiate among great apes, modern humans, and fossil hominid taxa.
Subject(s)
Hominidae/anatomy & histology , Mandible/anatomy & histology , Animals , Biological Evolution , Discriminant Analysis , Fossils , Hominidae/classification , Hominidae/embryology , Hominidae/genetics , Humans , Mandible/embryology , PhylogenyABSTRACT
During hominin evolution, an increase in the femoral bicondylar angle was the initial change that led to selection for protuberance of the lateral trochlear lip and the elliptical profile of the lateral condyle. No correlation is found during ontogeny between the degree of femoral obliquity and of the prominence of the lateral trochlear lip. Might there be a relationship with the elliptical profile of the lateral condyle? On intact femoral diaphyses of juvenile humans and great apes, we compared the anteroposterior length of the lateral and medial sides of the distal metaphysis. The two diaphyseal pillars remain equal during postnatal growth in great apes, while the growth of the lateral pillar far exceeds that of the medial pillar in humans. Increase in bicondylar angle is correlated with disproportionate anteroposterior lengthening of the lateral pillar. The increased anteroposterior length of the lateral side of the metaphysis would contribute to increasing the radius of the curvature of the lateral condyle, but not to the projection of the lateral trochlear lip. The similar neonatal and adult femoro-patellar joint shape in humans prompted an assessment of the similarity during growth of the entire neonatal and adult epiphyses. We showed that the entire epiphysis undergoes drastic changes in proportions during postnatal growth. Finally, we emphasize the need to distinguish the cartilaginous phenotype and the ossified phenotype of the distal femoral epiphysis (and of any epiphysis) during postnatal growth. This crucial distinction applies to most postcranial bones, for they almost all develop following the process of endochondral ossification.
Subject(s)
Biological Evolution , Cartilage, Articular/growth & development , Femur/growth & development , Hominidae/growth & development , Adaptation, Physiological , Adolescent , Animals , Cartilage, Articular/anatomy & histology , Cartilage, Articular/embryology , Child , Child, Preschool , Female , Femur/anatomy & histology , Femur/embryology , Hominidae/anatomy & histology , Hominidae/embryology , Humans , Infant , Infant, Newborn , Male , Phenotype , Phylogeny , Regression Analysis , Selection, GeneticSubject(s)
Brain/embryology , Evolution, Molecular , Hominidae/genetics , Animals , Genome, Human , Hominidae/embryology , Humans , Mice , PhylogenyABSTRACT
This study investigates whether macaques and humans possess a common pattern of relative growth during the fetal period. The fetal samples consist of 16 male pigtailed macaques (mean age, 20.5 gestational weeks) and 17 humans (9 males and 8 females; mean age, 29.5 gestational weeks). For each individual, three-dimensional coordinates of 18 landmarks on the skull were collected from three-dimensional computed tomographic (CT) reconstructed images and two-dimensional CT axial slices. Early and late groups were created from the human (early mean age, 24 weeks, N = 8; late mean age, 34 weeks, N = 9) and macaque samples (early mean age, 17.7 weeks, N = 7; late mean age, 23 weeks, N = 9). Inter- and intraspecific comparisons were made between the early and late groups. To determine if macaques and humans share a common fetal pattern of relative growth, human change in shape estimated from a comparison of early and late groups was compared to the pattern estimated between early and late macaque groups. Euclidean distance matrix analysis was used in all comparisons. Intraspecific comparisons indicate that the growing fetal skull displays the greatest amount of change along mediolateral dimensions. Changes during human growth are primarily localized to the basicranium and palate, while macaques experience localized change in the midface. Interspecific comparisons indicate that the two primate species do not share a common pattern of relative growth, and the macaque pattern is characterized by increased midfacial growth relative to humans. Our results suggest that morphological differences in the craniofacial skeleton of these species are in part established by differences in fetal growth patterns.
Subject(s)
Cephalometry/methods , Hominidae/embryology , Macaca nemestrina/embryology , Skull/embryology , Tomography, X-Ray Computed/methods , Anatomy, Comparative/methods , Animals , Craniology , Facial Bones/embryology , Female , Humans , Image Processing, Computer-Assisted/methods , Male , Prognathism/embryology , Skull Base/embryologyABSTRACT
The superior part of the ganglionic eminence has been shown to act as an intermediate target for outgrowing axons of projections between the thalamus and the cerebral cortex. This study aims at investigating whether amygdaloid projections transiently contact the inferior portion of the human ganglionic eminence which directly borders upon the amygdala. Between 16 and 20 weeks of gestation a high number of small fiber bundles which were immunolabelled with anti-MAP1b and anti-SNAP-25 could be traced from the amygdala towards the mantle zone of the ganglionic eminence. These fiber bundles left a fiber system which coursed from the amygdala towards the entorhinal cortex. Within the mantle zone of the ganglionic eminence immunoreactive puncta indicative of fiber termination were observed. After 22 weeks of gestation the number of fibers entering the ganglionic eminence gradually decreased. These results provide the first evidence that the marginal zone of the inferior ganglionic eminence is likely to constitute an intermediate target for growing axons which belong the amygdaloid projection to the entorhinal cortex.
Subject(s)
Amygdala/embryology , Cell Differentiation/physiology , Entorhinal Cortex/embryology , Fetus/embryology , Growth Cones/ultrastructure , Hominidae/embryology , Neural Pathways/embryology , Amygdala/cytology , Animals , Body Patterning/physiology , Entorhinal Cortex/cytology , Fetus/cytology , Growth Cones/metabolism , Humans , Immunohistochemistry , Membrane Proteins/metabolism , Microtubule-Associated Proteins/metabolism , Nerve Tissue Proteins/metabolism , Neural Pathways/cytology , Synaptosomal-Associated Protein 25ABSTRACT
The nasal floor structures in catarrhine primates have been studied on the basis of histological serial sections of older fetuses of Presbytis, Hylobates, Gorilla, Pan, Pongo and Homo. For outgroup comparisons, sections of the strepsirhine Daubentonia and the platyrrhine Callimico are presented; in these taxa the nasal floor cartilages are intimately connected not only with the nasopalatine duct (STENO) but also with the persisting vomeronasal organ (JACOBSON). Whereas the vomeronasal organ has disappeared as a functioning sensory organ in catarrhines (occasional embryonic vestiges are reported), the nasopalatine duct is retained in cercopithecoids, hylobatids and in Gorilla; in Pan, Pongo and Homo at least remnants of the duct and of the associated cartilages are preserved. The systematic meanings of these findings have been discussed.
Subject(s)
Cercopithecidae/embryology , Nasal Cavity/embryology , Palate/embryology , Animals , Cartilage/embryology , Gorilla gorilla/embryology , Hominidae/embryology , Humans , Hylobates/embryology , Pan troglodytes/embryology , Pongo pygmaeus/embryologyABSTRACT
This study examines the appearance of the secondary ossification centers in the lower arms, wrists, lower legs, and ankles of a cross-sectional sample of 20 infant orangutans and chimpanzees (15 of known age). The number of tarsal and carpal centers is analyzed relative to the degree of M1 development and the weight of individual animals. Variation in the appearance of these ossification centers is discussed relative to these variables and others. In addition, a sequence of appearance is established for the carpal and tarsal ossification centers in the orangutan and data is presented on the status of these centers in a fetal and newborn gorilla. Study results indicate that 1) there is variation in the number of secondary epiphyses present in animals of similar ages; 2) tarsal ossification is completed prior to carpal ossification in the orangutan; 3) there are indications of a relationship between weight and the number of ossification centers present in animals of similar age; and 4) there appears to be no evidence of specific relationships between carpal and tarsal development and M1 development.
Subject(s)
Arm/growth & development , Bone Development/physiology , Carpus, Animal/growth & development , Leg/growth & development , Pan troglodytes/growth & development , Pongo pygmaeus/growth & development , Tarsus, Animal/growth & development , Tooth/growth & development , Animals , Animals, Newborn/growth & development , Animals, Newborn/physiology , Carpal Bones/diagnostic imaging , Carpal Bones/growth & development , Female , Hominidae/embryology , Hominidae/growth & development , Humans , Male , Pan troglodytes/embryology , Pongo pygmaeus/embryology , Radiography , Tarsal Bones/diagnostic imaging , Tarsal Bones/growth & developmentABSTRACT
Human leg and foot anlagen of different developmental stages were studied by means of light and scanning electron microscopy. The findings were compared with principles of human arm and hand development and results obtained experimentally from chicken limbs. The limbs studied have in common the shaping, cell differentiation, and spatial arrangement of different cells as basic processes of development. On the other hand, upper and lower limbs are very different in human and avian embryos with regard to their position, form, and function. We found that the different positions in relation to the dorsal and ventral surfaces and maintenance of the apical ectodermal ridge (AER) are important factors leading to the different orientations and forms of limbs. The unequal length of the fingers and toes might also be explained in this way. Differences in the position of the most distal muscles in the hand and foot could be a consequence of the cranio-caudal sequence of development. The factors controlling the developmental differences between arm and leg are discussed.
Subject(s)
Embryonic and Fetal Development , Foot/embryology , Hominidae/embryology , Leg/embryology , Animals , Embryo, Mammalian/anatomy & histology , Fetus/anatomy & histology , Gestational Age , HumansABSTRACT
A number of morphological particularities of humans, generally thought to be specializations produced by natural selection, arguably are instances of hypermorphosis: alterations in proportion brought about by simple prolongation of general embryonic allometries. The descended larynx, the flattened human chest, and several limb proportions are given as examples. The case of the human foot, often quoted as an example of advanced specialization in humans, is examined in some more detail. Besides, it is argued that the human growth pattern displays a unique 7-year periodicity unlikely to be the result of the erratics of Darwinian evolution. Developmental acceleration is the unavoidable correlate of animal specialization; it brings about the breakdown of the periodicity present in the generalized humanlike development and causes the embryonic allometries to be cut off prematurely in the non-human mammal.
Subject(s)
Hominidae/anatomy & histology , Intellectual Disability/etiology , Adult , Animals , Biological Evolution , Foot/anatomy & histology , Foot/growth & development , History, 20th Century , Hominidae/embryology , Hominidae/growth & development , Humans , Infant, Newborn , Intellectual Disability/history , Larynx/anatomy & histology , Larynx/embryology , Larynx/growth & development , Models, Biological , Primates/anatomy & histology , Primates/embryology , Thorax/anatomy & histology , Thorax/embryology , Thorax/growth & developmentABSTRACT
Insights into the programmatic induction of neuronal and glial genes during human embryogenesis have depended largely on extrapolations of data derived from experimental mammals. However, the assumptions upon which these extrapolations are based have not been rigorously tested. Indeed, practically no information is available even on the human counterparts of the relatively small subset of well-characterized, developmentally regulated neuron and glial specific genes of the mammalian CNS. Thus, the developmental programs upon which human neural embryogenesis are based remain largely undeciphered. We have addressed this problem in immunohistochemical studies conducted on 22 human fetal spinal cords with gestational ages (GAs) that ranged from 6 to 40 weeks by using monoclonal antibodies to several classes of neuron or glial specific polypeptides. These polypeptides included: representatives of four different types (Types I-IV) of intermediate filament proteins, i.e., vimentin filament protein (VFP), glial fibrillary acidic protein (GFAP), different phospho-isoforms of the high (NF-H), middle (NF-M), and low (NF-L) molecular weight (Mr) neurofilament (NF) subunits, both acidic and basic cytokeratin (CK) proteins; three different microtubule associated proteins (MAPs), i.e., MAP2, MAP5, and tau; two different synaptic or coated vesicle proteins, i.e., synaptophysin (SYP) and clathrin light chain B (LCb); an oligodendroglial specific protein, i.e., myelin basic protein (MBP); and a receptor for a CNS trophic factor, i.e., the nerve growth factor receptor (NGFR).(ABSTRACT TRUNCATED AT 400 WORDS)
Subject(s)
Hominidae/embryology , Intermediate Filament Proteins/analysis , Neuroglia/physiology , Neurons/physiology , Spinal Cord/embryology , Animals , Axons/physiology , Embryo, Mammalian , Female , Fetus , Gestational Age , Humans , Immunohistochemistry , Infant, Newborn , Neuroglia/cytology , Neurons/cytology , Phenotype , Pregnancy , Spinal Cord/cytologyABSTRACT
Possible etiological factors of congenital malformations as well as of human trisomies are considered in the framework of the repressor hypothesis. In this approach gene expression is envisaged from the point of view of the functional variations of the total activation energy for normal gene expression in homeostatic equilibrium. We restrict our attention to variations of the total activation energy under the effect of temperature gradients. We discuss the evidence that hyperthermia may be an etiological factor for trisomies in humans.
