Vocal cords

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Vocal folds
Gray956.png
Laryngoscopic view of the vocal folds.
Illu07 larynx02.jpg
Details
Precursor Sixth pharyngeal arch
System Respiratory system
Identifiers
Latin plica vocalis
MeSH D014827
TA A06.2.09.013
FMA 55457
Anatomical terminology
Vocal folds (open)
Vocal folds (speaking)

The vocal folds, also known commonly as vocal cords, are composed of twin infoldings of mucous membrane stretched horizontally, from back to front, across the larynx. They vibrate, modulating the flow of air being expelled from the lungs during phonation.[1][2][3]

Open when breathing and vibrating for speech or singing, the folds are controlled via the vagus nerve.

Structure[edit]

The vocal folds are located within the larynx at the top of the trachea, they are attached posteriorly to the arytenoid cartilages, and anteriorly to the thyroid cartilage. They are part of the glottis which includes the rima glottidis, their outer edges are attached to muscle in the larynx while their inner edges, or margins, are free forming the opening called the rima glottidis. They are constructed from epithelium, but they have a few muscle fibres in them, namely the vocalis muscle which tightens the front part of the ligament near to the thyroid cartilage, they are flat triangular bands and are pearly white in color. Above both sides of the glottis are the two vestibular folds or false vocal folds which have a small sac between them.

Situated above the larynx, the epiglottis acts as a flap which closes off the trachea during the act of swallowing to direct food into the esophagus. If food or liquid does enter the trachea and contacts the vocal folds it causes a cough reflex to expel the matter in order to prevent pulmonary aspiration.

Variations[edit]

Males and females have different vocal fold sizes. Adult male voices are usually lower pitched due to longer and thicker folds, the male vocal folds are between 1.75 cm and 2.5 cm (approx 0.75" to 1.0") in length,[2] while female vocal folds are between 1.25 cm and 1.75 cm (approx 0.5" to 0.75") in length. The vocal folds of children are much shorter than those of adult males and females, the difference in vocal fold length and thickness between males and females causes a difference in vocal pitch. Additionally, genetic factors cause variations between members of the same sex, with males' and females' voices being categorized into voice types.

False vocal folds[edit]

Main article: Vestibular fold

The vocal folds are sometimes called 'true vocal folds' to distinguish them from the 'false vocal folds' known as vestibular folds or ventricular folds, these are a pair of thick folds of mucous membrane that protect and sit slightly superior to the more delicate true folds. They have a minimal role in normal phonation, but are often used to produce deep sonorous tones in Tibetan chant and Tuvan throat singing,[4] as well as in musical screaming and the death growl vocal style.[citation needed]

Microanatomy[edit]

Main article: Histology of the vocal folds

Mature human vocal folds are composed of layered structures which are quite different at the histological level, the topmost layer comprises stratified squamous epithelium which is bordered by ciliated pseudostratified epithelium. The inner lining surface of this squamous epithelium is covered by a layer of mucus (acting as a mucociliary clearance), which is composed of two layers: a mucinous layer and serous layer. Both mucus layers provide viscous and watery environment for cilia beating posteriorally and superiorly, the mucociliary clearance keeps the vocal folds essentially moist and lubricated.[5] The epidermis layer is secured to the deeper connective tissue by basement membrane. Due to the primarily amorphous fibrous and nonfibrous proteins in the lamina propria, the basement membrane applies strong anchoring filaments like collagen Ⅳ and Ⅶ to secure the hemidesmosome of basal cell to the lamina propria. These attachments are strong enough to sustain beating and stretch, to which VFs are subjected,[5] the population density of some of the anchoring fibers in the basement membrane, such as collagen Ⅶ, is genetically determined, and these genetics may influence the health and pathogenesis of the vocal folds.[6]

Larynx showing vocal ligaments

The next three layers comprise lamina of lipopolysaccharides (LPs), which are stratified by their histological composition of elastin and collagen fibers, with fibroblast, myofibroblast and macrophages interspersed sparsely,[5] the superficial layer LPs (SLLPs), also known as Reinke's space, is composed of amorphous substance and microfibrils[7] which allows this cover layer to “slide” over the deep layer easily.[8] The vibratory and viscoelastic characteristics of human VFs are mainly attributed to the molecular composition of SLLPs; in normal vocal fold, the jelly-like “Reinke's space” is very loose and abundant with interstitial proteins such as hyaluronic acid, fibronectin, proteoglycan like fibromodulin, decorin and versican. All these ECM components together regulate the water content of vocal fold and render the viscous shear property for it.[9][10] The squamous epithelium and superficial lamina propria form the vocal mucosa which serves as vibratory component in phonation, the mucosa layer vibrates at a frequency range of 100–1000 Hz and displacement at 1mm approximately.[11] The intermediate layer of LPs consists primarily of elastic fiber while the deep layer LP consists of fewer elastin and more collagen fibers, these two layers have poor differentiated boundary but are increasingly stiffer than SLLPs. The intermediate and deep layers of LPs compose the vocal ligaments which are enclosed within the vocal folds and are responsible for strain in phonation. Within the ECM community of vocal ligament, fibrous proteins such as elastin and collagen are pivotal in maintaining the proper elastic biomechanical property of vocal fold.[8] Elastin fibers impart the flexibility and elasticity of the vocal folds and, collagen is responsible for the resistance and resiliece to tensile strength,[12] the normal strain level of vocal ligament ranges from 0–15% during phonation[8] These fibrous proteins exhibit distribution variations spatially and temporally due to fibroblast turnover during tissue maturation and aging,[7][13] each vocal ligament is a band of yellow elastic tissue attached in front to the angle of the thyroid cartilage, and behind to the vocal process of the arytenoid cartilage.

Development[edit]

In newborns[edit]

Newborns have a uniform monolayered lamina propria, which appears loose with no vocal ligament,[14] the monolayered lamina propria is composed of ground substances such as hyaluronic acid and fibronectin, fibroblasts, elastic fibers, and collagenous fibers. While the fibrous components are sparse, making the lamina propria structure loose, the hyaluronic acid (HA) content is high.

HA is a bulky, negatively charged glycosaminoglycan, whose strong affinity with water procures HA its viscoelastic and shock absorbing properties essential to vocal biomechanics.[15] Viscosity and elasticity are critical to voice production. Chan, Gray and Titze, quantified the effect of HA on both the viscosity and the elasticity of vocal folds (VF) by comparing the properties of tissues with and without HA,[16] the results showed that removal of HA decreased the stiffness of VF by an average of 35%, but increased their dynamic viscosity by an average of 70% at frequencies higher than 1 Hz. Newborns have been shown to cry an average of 6.7 hours per day during the first 3 months, with a sustained pitch of 400–600 Hz, and a mean duration per day of 2 hours.[17] Similar treatment on adult VF would quickly result in edema, and subsequently aphonia. Schweinfurth and al. presented the hypothesis that high hyaluronic acid content and distribution in newborn VF is directly associated with newborn crying endurance.[17] These differences in newborn vocal fold composition would also be responsible for newborns inability to articulate sounds, besides the fact that their lamina propria is a uniform structure with no vocal ligament, the layered structure necessary for phonation will start to develop during the infancy and until the adolescence.[14]

The fibroblasts in the newborn Reinke's space are immature, showing an oval shape, and a large nucleus-cytoplasm ratio,[14] the rough endoplasmic reticulum and Golgi apparatus, as shown by electron micrographs, are not well developed, indicating that the cells are in a resting phase. The collagenous and reticular fibers in the newborn VF are fewer than in the adult one, adding to the immaturity of the vocal fold tissue.

In the infant, many fibrous components were seen to extend from the macula flava towards the Reinke's space. Fibronectin is very abundant in the Reinke's space of newborn and infant. Fibronectin is a glycoprotein that is believed to act as a template for the oriented deposition of the collagen fibers, stabilizing the collagen fibrils. Fibronectin also acts as a skeleton for the elastic tissue formation.[14] Reticular and collagenous fibers were seen to run along the edges of the VF throughout the entire lamina propria.[14] Fibronectin in the Reinke's space appeared to guide those fibers and orient the fibril deposition, the elastic fibers remained sparse and immature during infancy, mostly made of microfibrils. The fibroblasts in the infant Reinke's space were still sparse but spindle-shaped, their rough endoplasmic reticulum and Golgi apparatus were still not well developed, indicating that despite the change in shape, the fibroblasts still remained mostly in a resting phase. Few newly released materials were seen adjacent to the fibroblasts, the ground substance content in the infant Reinke's space seemed to decrease over time, as the fibrous component content increased, thus slowly changing the vocal fold structure.

In adults[edit]

Human VF are paired structures located in the larynx, just above the trachea, which vibrate and are brought in contact during phonation, the human VF are roughly 12 – 24 mm in length, and 3–5 mm thick.[18] Histologically, the human VF are a laminated structure composed of five different layers, the vocalis muscle, main body of the VF, is covered by the mucosa, which consists of the epithelium and the lamina propria.[19] The latter is a pliable layer of connective tissue subdivided into three layers: the superficial layer (SLP), the intermediate layer (ILP), and the deep layer (DLP).[5] Layer distinction is either made looking at differential in cell content or extracellular matrix (ECM) content, the most common way being to look at the ECM content. The SLP has fewer elastic and collagenous fibers than the two other layers, and thus is looser and more pliable, the ILP is mostly composed of elastic fibers, while the DLP has fewer elastic fibers, and more collagenous fibers.[19] In those two layers, which form what is known as the vocalis ligament, the elastic and collagenous fibers are densely packed as bundles that run almost parallel to the edge of the vocal fold.[19]

The extracellular matrix of the VF LP is composed of fibrous proteins such as collagen and elastin, and interstitial molecules such as HA, a non-sulfated glycosaminoglycan.[5] While the SLP is rather poor in elastic and collagenous fibers, the ILP and DLP are mostly composed of it, with the concentration of elastic fibers decreasing and the concentration of collagenous fibers increasing as the vocalis muscle is approached.[19] Fibrous proteins and interstitial molecules play different roles within the ECM. While collagen (mostly type I) provides strength and structural support to the tissue, which are useful to withstanding stress and resisting deformation when subjected to a force, elastin fibers bring elasticity to the tissue, allowing it to return to its original shape after deformation.[5] Interstitial proteins, such as HA, plays important biological and mechanical roles in the VF tissue;[15] in the VF tissue, HA plays a role of shear-thinner, affecting the tissue viscosity, space-filler, shock absorber, as well as wound healing and cell migration promoter. The distribution of those proteins and interstitial molecules has been proven to be affected by both age and gender, and is maintained by the fibroblasts.[5][9][15][20]

Maturation[edit]

Vocal fold structure in adults is quite different from that in newborns. Exactly how the VF mature from an immature monolayer in newborns to a mature three layer tissue in adults is still unknown, however a few studies have investigated the subjects and brought some answers.

Hirano et al. previously found that the newborns did not have a true lamina propria, but instead had cellular regions called maculae flavae, located at the anterior and posterior ends of the loose vocal fold tissue.[14][21] Boseley and Hartnick examined at the development and maturation of pediatric human vocal fold lamina propria.[22] Hartnick was the first one to define each layer by a change in their cellular concentration,[23] he also found that the lamina propria monolayer at birth and shortly thereafter was hypercellular, thus confirming Hirano’s observations. By 2 months of age, the vocal fold started differentiating into a bilaminar structure of distinct cellular concentration, with the superficial layer being less densely populated than the deeper layer. By 11 months, a three-layered structure starts to be noted in some specimens, again with different cellular population densities, the superficial layer is still hypocellular, followed by an intermediate more hypercellular layer, and a deeper hypercellular layer, just above the vocalis muscle. Even though the VF seem to start organizing, this is not representative of the trilaminar structure seen in adult tissues, where the layer are defined by their differential elastin and collagen fiber compositions. By 7 years of age, all specimens show a three-layered vocal fold structure, based on cellular population densities, at this point, the superficial layer was still hypocellular, the middle layer was the hypercellualr one, with also a greater content of elastin and collagen fibers, and the deeper layer was less cellularly populated. Again, the distinction seen between the layers at this stage is not comparable to that seen in the adult tissue, the maturation of the VF did not appear before 13 years of age, where the layers could be defined by their differential fiber composition rather than by their differential cellular population. The pattern now show a hypocellular superficial layer, followed by a middle layer composed predominantly of elastin fiber, and a deeper layer composed predominantly of collagen fibers, this pattern can be seen in older specimens up to 17 years of age, and above. While this study offers a nice way to see the evolution from immature to mature VF, it still does not explain what is the mechanism behind it.

Macula flavae[edit]

Maculae flavae are located at the anterior and posterior ends of the membranous parts of the VF,[24] the histological structure of the macula flava is unique, and Sato and Hirano speculated that it could play an important role in growth, development and aging of VF. The macula flava is composed of fibroblasts, ground substances, elastic and collagenous fibers. Fibroblasts were numerous and spindle or stellate-shaped, the fibroblasts have been observed to be in active phase, with some newly released amorphous materials present at their surface. From a biomechanical point of view, the role of the macula flava is very important. Hirano and Sato studies suggested that the macula flava is responsible for the synthesis of the fibrous components of the VF. Fibroblasts have been found mostly aligned in the direction of the vocal ligament, along bundles of fibers, it then was suggested that the mechanical stresses during phonation were stimulating the fibroblasts to synthesize those fibers.

Impact of phonation[edit]

The viscoelastic properties of human vocal fold lamina propria are essential for their vibration, and depend on the composition and structure of their extracellular matrix (ECM). Adult VF have a layered structure which is based on the layers differential in ECM distribution. Newborns on the other hand, do not have this layered structure, their VF are uniform, and immature, making their viscoelastic properties most likely unsuitable for phonation. HA plays a very important role in the vocal fold biomechanics. In fact, HA has been described as the ECM molecule that not only contributes to the maintenance of an optimal tissue viscosity that allows phonation, but also of an optimal tissue stiffness that allows frequency control.[16] CD44 is a cell surface receptor for HA. Cells such as fibroblasts are responsible for synthesizing ECM molecules. Cell surface matrix receptors in return, feed back to the cells through cell-matrix interaction, allowing the cell to regulate its metabolism.

Sato et al.[25] carried out a histopathologic investigation of unphonated human VF. Vocal fold mucosae, which were unphonated since birth, of three young adults (17, 24, and 28 years old) were looked at using light and electron microscopy, the results show that the vocal fold mucosae were hypoplastic, and rudimentary, and like newborns, did not have any vocal ligament, Reinke's space, or layered structure. Like newborns, the lamina propria appeared as a uniform structure, some stellate cells were present in the macula flava, but started to show some signs of degeneration. The stellate cells synthesized fewer ECM molecules, and the cytoplasmic processes were shown to be short and shrinking, suggesting a decreased activity, those results confirm the hypothesis that phonation stimulates stellate cells into producing more ECM.

Furthermore, using a specially designed bioreactor, Titze et al. showed that fibroblasts exposed to mechanical stimulation have differing levels of ECM production from fibroblasts that are not exposed to mechanical stimulation.[26] The gene expression levels of ECM constituents such as fibronectin, MMP1, decorin, fibromodulin, HA synthase 2, and CD44 were altered. All those genes are involved in ECM remodeling, thus suggesting that mechanical forces applied to the tissue, alter the expression levels of ECM related genes, which in turn allow the cells present in the tissue to regulate the ECM constituent synthesis, thus affecting the tissue’s composition, structure, and biomechanical properties; in the end, cell-surface receptors close the loop by giving feedback on the surrounding ECM to the cells, affecting also their gene expression level.

Impact of hormones[edit]

Other studies suggest that hormones play also an important role in vocal fold maturation. Hormones are molecules secreted into the blood stream to be delivered at different targeted sites, they usually promote growth, differentiation and functionality in different organs or tissues. Their effect is due to their ability to bind to intracellular receptors, modulating the gene expression, and subsequently regulating protein synthesis,[27] the interaction between the endocrine system and tissues such as breast, brain, testicles, heart, bones, etc., is being extensively studied. It has clearly been seen that the larynx is somewhat affected by hormonal changes, but surprisingly, very few studies are working on elucidating this relationship, the effect of hormonal changes in voice is clearly seen when hearing male and female voices, or when listening to a teenage voice changing during puberty. Actually, it is believed that the number of hormonal receptors in the pre-pubertal phase is higher than in any other age.[27] Menstruation has also been seen to influence the voice; in fact, singers are encouraged by their instructors not to perform during their pre-menstrual period, because of a drop in their voice quality.[27]

Vocal fold phonatory functions are known to change from birth to old age, the most significant changes occur in development between birth and puberty, and in old age.[19][28] Hirano et al. previously described several structural changes associated with aging, in the vocal fold tissue.[29] Some of those changes are: a shortening of the membranous vocal fold in males, a thickening of the vocal fold mucosa and cover in females, and a development of edema in the superficial lamina propria layer in both sexes. Hammond et al. observed that the HA content in the vocal fold lamina propria was significantly higher in males than in females.[9] Although all those studies did show that there are clear structural and functional changes seen in the human VF which are associated with gender and age, none really fully elucidated the underlying cause of those changes; in fact, only a few recent studies started to look at the presence and role of hormone receptors in the VF. Newman et al. found that hormone receptors are indeed present in the VF, and show a statistical distribution difference with respect to age and gender.[28] They have identified the presence of androgen, estrogen, and progesterone receptors in epithelial cells, granular cells and fibroblasts of VF, suggesting that some of the structural changes seen in the VF could be due to hormonal influences.[28] In this specific study, androgen and progesterone receptors were found more commonly in males than in females; in others studies, it has been suggested that the estrogen/androgen ratio be partly responsible for the voice changes observed at menopause.[30] As previously said, Hammond et al. showed than the HA content was higher in male than in female VF. Bentley et al. demonstrated that sex skin swelling seen in monkey was due to an increase in HA content, which was in fact mediated by estrogen receptors in dermal fibroblasts.[31] An increase in collagen biosynthesis mediated by the estrogen receptors of dermal fibroblasts was also observed. A connection between hormone levels, and ECM distribution in VF depending on age and gender could be made. More particularly a connection between higher hormone levels and higher HA content in males could exist in the human vocal fold tissue, although a relationship between hormone levels and ECM biosynthesis in vocal fold can be established, the details of this relationship, and the mechanisms of the influence has not been elucidated yet.

Function[edit]

Oscillation[edit]

The vocal folds in motion.

The larynx is a major (but not the only) source of sound in speech, generating sound through the rhythmic opening and closing of the vocal folds. To oscillate, the vocal folds are brought near enough together such that air pressure builds up beneath the larynx. The folds are pushed apart by this increased subglottal pressure, with the inferior part of each fold leading the superior part, such a wave-like motion causes a transfer of energy from the airflow to the fold tissues.[32] Under the correct conditions, the energy transferred to the tissues is large enough to overcome losses by dissipation and the oscillation pattern will sustain itself. In essence, sound is generated in the larynx by chopping up a steady flow of air into little puffs of sound waves.[33] (video)

The perceived pitch of a person's voice is determined by a number of different factors, most importantly the fundamental frequency of the sound generated by the larynx. The fundamental frequency is influenced by the length, size, and tension of the vocal folds. This frequency averages about 125 Hz in an adult male, 210 Hz in adult females, and over 300 Hz in children. Depth-kymography[34] is an imaging method to visualize the complex horizontal and vertical movements of vocal folds.

The vocal folds generate a sound rich in harmonics. The harmonics are produced by collisions of the vocal folds with themselves, by recirculation of some of the air back through the trachea, or both,[35] some singers can isolate some of those harmonics in a way that is perceived as singing in more than one pitch at the same time—a technique called overtone singing or throat singing such as in the tradition of Tuvan throat singing.

Clinical significance[edit]

Wound healing[edit]

Wound healing is a natural regeneration process of dermal and epidermal tissue involving a sequence of biochemical events, these events are complex and can be categorized into three stages: inflammation, proliferation and tissue remodeling.[36] The study on vocal fold wound healing is not as extensive as that on animal models due to the limited availability of human vocal folds. Vocal fold injuries can have a number of causes including chronic overuse, chemical, thermal and mechanical trauma such as smoking, laryngeal cancer, and surgery. Other benign pathological phenomena like polyps, vocal fold nodules and edema will also introduce disordered phonation.[37]

Any injury to human vocal folds elicits a wound healing process characterized by disorganized collagen deposition and, eventually, formation of scar tissue.[38][39][40][41] Verdolini[42] and her group sought to detect and describe acute tissue response of injured rabbit VF model. They quantified the expression of two biochemical markers: interleukin 1 and prostaglandin E2, which are associated with acute wound healing, they found the secretions of these inflammatory mediators were significantly elevated when collected from injured VF versus normal VF. This result was consistent with their previous study about the function of IL-1 and PGE-2 in wound healing.[42][43] Investigation about the temporal and magnitude of inflammatory response in VFs may benefit for elucidating subsequent pathological events in vocal fold wounding,[43] which is good for clinician to develop therapeutic targets to minimize scar formation. In the proliferative phase of VFs wound healing, if the production of HA and collagen is not balanced, which means the HA level is lower than normal, the fibrosis of collagen cannot be regulated. Consequently, regenerative-type wound healing turns to be the formation of scar.[38][41] Scarring may lead to the deformity of vocal fold edge, the disruption of LPs viscosity and stiffness.[44] Patients suffering from vocal fold scar complain about increased phonatory effort, vocal fatigue, breathlessness, and dysphonia.[38] Vocal fold scar is one of the most challenging problems for otolaryngologists because it’s hard to be diagnosed at germinal stage and the function necessity of VF is delicate.

Terminology[edit]

The vocal folds are commonly referred to as vocal cords, and less commonly as vocal flaps or vocal bands, the term vocal cords was coined by the French anatomist Antoine Ferrein in 1741. In his violin analogy of the human voice, he postulated that the moving air acted like a bow on cordes vocales,[45] the alternative spelling in English is vocal chords, possibly due to the musical connotations or to confusion with the geometrical definition of the word chord. While both spellings have historical precedents, standard American spelling is cords.[46] According to the Oxford English Corpus, a database of 21st-century texts that contains everything from academic journal articles to unedited writing and blog entries, contemporary writers opt for the nonstandard chords instead of cords 49% of the time.[47][48] The cords spelling is also standard in the United Kingdom and Australia.

In phonetics, vocal folds is preferred over vocal cords, on the grounds that it is more accurate and illustrative.[49][50][51]

See also[edit]

This article uses anatomical terminology; for an overview, see Anatomical terminology.

Additional images[edit]

  • Vocal folds.

  • Coronal section of larynx and upper part of trachea.

  • The entrance to the larynx, viewed from behind.

  • Muscles of the larynx, seen from above.

References[edit]

  1. ^ Titze IR (January 2008). "The human instrument". Sci. Am. 298 (1): 94–101. doi:10.1038/scientificamerican0108-94. PMID 18225701. 
  2. ^ a b Titze, Ingo R. (1994). Principles of Voice Production. Prentice Hall. ISBN 978-0-13-717893-3. Archived from the original on 2017-09-05. 
  3. ^ Maton, Anthea; Hopkins, Jean; McLaughlin, Charles William; Johnson, Susan; Warner, Maryanna Quon; LaHart, David; Wright, Jill D. (1993). Human Biology and Health. Prentice Hall. ISBN 0-13-981176-1. 
  4. ^ Fuks, Leonardo (1998). "From Air to Music: Acoustical, Physiological and Perceptual Aspects of Reed Wind Instrument Playing and Vocal-Ventricular Fold Phonation". Stockholm, Sweden. Archived from the original on 2009-12-27. Retrieved 2010-01-05. 
  5. ^ a b c d e f g Gray SD (August 2000). "Cellular physiology of the vocal folds". Otolaryngol. Clin. North Am. 33 (4): 679–98. PMID 10918654. 
  6. ^ Briggaman RA, Wheeler CE (August 1975). "Epidermolysis bullosa dystrophica-recessive: a possible role of anchoring fibrils in the pathogenesis". J. Invest. Dermatol. 65 (2): 203–11. doi:10.1111/1523-1747.ep12598208. PMID 1151111. 
  7. ^ a b Sato K, Hirano M (January 1997). "Age-related changes of elastic fibers in the superficial layer of the lamina propria of vocal folds". Ann. Otol. Rhinol. Laryngol. 106 (1): 44–8. doi:10.1177/000348949710600109. PMID 9006361. 
  8. ^ a b c Linda Rammage; M D Morrison; Hamish Nichol, Management of the voice and its disorders, published by:: Singular/Thomson Learning, San Diego, CA ,2001, 269–270.
  9. ^ a b c Hammond TH, Zhou R, Hammond EH, Pawlak A, Gray SD (March 1997). "The intermediate layer: a morphologic study of the elastin and hyaluronic acid constituents of normal human vocal folds". J Voice. 11 (1): 59–66. doi:10.1016/s0892-1997(97)80024-0. PMID 9075177. 
  10. ^ Pawlak AS, Hammond T, Hammond E, Gray SD (January 1996). "Immunocytochemical study of proteoglycans in vocal folds". Ann. Otol. Rhinol. Laryngol. 105 (1): 6–11. PMID 8546427. 
  11. ^ Hirano, M; Kakita, Y (1985). "Cover-body theory of vocal fold vibration". In Daniloff, Raymond. Speech science: recent advances. Speech, language, and hearing science. College-Hill Press. ISBN 978-0-933014-95-4. Archived from the original on 2017-09-05. 
  12. ^ Gray SD, Titze IR, Alipour F, Hammond TH (January 2000). "Biomechanical and histologic observations of vocal fold fibrous proteins". Ann. Otol. Rhinol. Laryngol. 109 (1): 77–85. doi:10.1177/000348940010900115. PMID 10651418. 
  13. ^ Sato K, Hirano M, Nakashima T (January 2002). "Age-related changes of collagenous fibers in the human vocal fold mucosa". Ann. Otol. Rhinol. Laryngol. 111 (1): 15–20. doi:10.1177/000348940211100103. PMID 11800365. 
  14. ^ a b c d e f Sato K, Hirano M, Nakashima T (May 2001). "Fine structure of the human newborn and infant vocal fold mucosae". Ann. Otol. Rhinol. Laryngol. 110 (5 Pt 1): 417–24. PMID 11372924. 
  15. ^ a b c Ward PD, Thibeault SL, Gray SD (September 2002). "Hyaluronic acid: its role in voice". J Voice. 16 (3): 303–9. doi:10.1016/s0892-1997(02)00101-7. PMID 12395982. 
  16. ^ a b Chan RW, Gray SD, Titze IR (June 2001). "The importance of hyaluronic acid in vocal fold biomechanics". Otolaryngol Head Neck Surg. 124 (6): 607–14. doi:10.1067/mhn.2001.115906. PMID 11391249. 
  17. ^ a b Schweinfurth JM, Thibeault SL (September 2008). "Does hyaluronic acid distribution in the larynx relate to the newborn's capacity for crying?". Laryngoscope. 118 (9): 1692–9. doi:10.1097/MLG.0b013e3181782754. PMID 18596477. 
  18. ^ Hahn MS, Teply BA, Stevens MM, Zeitels SM, Langer R (March 2006). "Collagen composite hydrogels for vocal fold lamina propria restoration". Biomaterials. 27 (7): 1104–9. doi:10.1016/j.biomaterials.2005.07.022. PMID 16154633. 
  19. ^ a b c d e Hirano, M., S. Kurita, and T. Nakashima. Vocal fold physiology : contemporary research and clinical issues. in Vocal Fold Physiology, Conference. 1981. San Diego, Calif.: College-Hill Press.
  20. ^ Hammond TH, Gray SD, Butler J, Zhou R, Hammond E (October 1998). "Age- and gender-related elastin distribution changes in human vocal folds". Otolaryngol Head Neck Surg. 119 (4): 314–22. doi:10.1016/s0194-5998(98)70071-3. PMID 9781983. 
  21. ^ Sato K, Hirano M (July 1995). "Histologic investigation of the macula flava of the human newborn vocal fold". Ann. Otol. Rhinol. Laryngol. 104 (7): 556–62. doi:10.1177/000348949510400710. PMID 7598369. 
  22. ^ Boseley ME, Hartnick CJ (October 2006). "Development of the human true vocal fold: depth of cell layers and quantifying cell types within the lamina propria". Ann. Otol. Rhinol. Laryngol. 115 (10): 784–8. doi:10.1177/000348940611501012. PMID 17076102. 
  23. ^ Hartnick CJ, Rehbar R, Prasad V (January 2005). "Development and maturation of the pediatric human vocal fold lamina propria". Laryngoscope. 115 (1): 4–15. doi:10.1097/01.mlg.0000150685.54893.e9. PMID 15630357. 
  24. ^ Sato K, Hirano M (February 1995). "Histologic investigation of the macula flava of the human vocal fold". Ann. Otol. Rhinol. Laryngol. 104 (2): 138–43. doi:10.1177/000348949510400210. PMID 7857016. 
  25. ^ Sato K, Nakashima T, Nonaka S, Harabuchi Y (June 2008). "Histopathologic investigations of the unphonated human vocal fold mucosa". Acta Otolaryngol. 128 (6): 694–701. doi:10.1080/00016480701675643. PMID 18568507. 
  26. ^ Titze IR, Hitchcock RW, Broadhead K, et al. (October 2004). "Design and validation of a bioreactor for engineering vocal fold tissues under combined tensile and vibrational stresses". J Biomech. 37 (10): 1521–9. doi:10.1016/j.jbiomech.2004.01.007. PMID 15336927. 
  27. ^ a b c Rios OA, Duprat Ade C, Santos AR (2008). "Immunohistochemical searching for estrogen and progesterone receptors in women vocal fold epithelia". Braz J Otorhinolaryngol. 74 (4): 487–93. PMID 18852972. Archived from the original on 2014-08-12. 
  28. ^ a b c Newman SR, Butler J, Hammond EH, Gray SD (March 2000). "Preliminary report on hormone receptors in the human vocal fold". J Voice. 14 (1): 72–81. doi:10.1016/s0892-1997(00)80096-x. PMID 10764118. 
  29. ^ Hirano M, Kurita S, Sakaguchi S (1989). "Ageing of the vibratory tissue of human vocal folds". Acta Otolaryngol. 107 (5–6): 428–33. doi:10.3109/00016488909127535. PMID 2756834. 
  30. ^ Nelson, J.F. (1995). "The potential role of selected endocrine systems in aging processes". Comprehensive Physiology. Wiley Online Library. doi:10.1002/cphy.cp110115. Archived from the original on 2014-08-09. 
  31. ^ Bentley JP, Brenner RM, Linstedt AD, et al. (November 1986). "Increased hyaluronate and collagen biosynthesis and fibroblast estrogen receptors in macaque sex skin". J. Invest. Dermatol. 87 (5): 668–73. doi:10.1111/1523-1747.ep12456427. PMID 3772161. 
  32. ^ Lucero, J.C. (1995). "The minimum lung pressure to sustain vocal fold oscillation". Journal of the Acoustical Society of America. 98: 779–784. doi:10.1121/1.414354. 
  33. ^ Titze IR (April 1988). "The physics of small-amplitude oscillation of the vocal folds". J. Acoust. Soc. Am. 83 (4): 1536–52. doi:10.1121/1.395910. PMID 3372869. 
  34. ^ George NA, de Mul FF, Qiu Q, Rakhorst G, Schutte HK (May 2008). "Depth-kymography: high-speed calibrated 3D imaging of human vocal fold vibration dynamics". Phys Med Biol. 53 (10): 2667–75. doi:10.1088/0031-9155/53/10/015. PMID 18443389. 
  35. ^ Ingo Titze, University of Iowa.
  36. ^ Stadelmann WK, Digenis AG, Tobin GR (August 1998). "Physiology and healing dynamics of chronic cutaneous wounds". Am. J. Surg. 176 (2A Suppl): 26S–38S. doi:10.1016/S0002-9610(98)00183-4. PMID 9777970. 
  37. ^ Wallis L, Jackson-Menaldi C, Holland W, Giraldo A (March 2004). "Vocal fold nodule vs. vocal fold polyp: answer from surgical pathologist and voice pathologist point of view". J Voice. 18 (1): 125–9. doi:10.1016/j.jvoice.2003.07.003. PMID 15070232. 
  38. ^ a b c Rosen CA (October 2000). "Vocal fold scar: evaluation and treatment". Otolaryngol. Clin. North Am. 33 (5): 1081–6. PMID 10984771. 
  39. ^ Hirano S, Bless DM, Rousseau B, et al. (March 2004). "Prevention of vocal fold scarring by topical injection of hepatocyte growth factor in a rabbit model". Laryngoscope. 114 (3): 548–56. doi:10.1097/00005537-200403000-00030. PMID 15091233. 
  40. ^ Peled ZM, Chin GS, Liu W, Galliano R, Longaker MT (October 2000). "Response to tissue injury". Clin Plast Surg. 27 (4): 489–500. PMID 11039884. 
  41. ^ a b Longaker MT, Chiu ES, Adzick NS, Stern M, Harrison MR, Stern R (April 1991). "Studies in fetal wound healing. V. A prolonged presence of hyaluronic acid characterizes fetal wound fluid". Ann. Surg. 213 (4): 292–6. doi:10.1097/00000658-199104000-00003. PMC 1358347Freely accessible. PMID 2009010. 
  42. ^ a b Branski RC, Rosen CA, Verdolini K, Hebda PA (January 2004). "Markers of wound healing in vocal fold secretions from patients with laryngeal pathology". Ann. Otol. Rhinol. Laryngol. 113 (1): 23–9. doi:10.1177/000348940411300105. PMID 14763567. 
  43. ^ a b Branski RC, Rosen CA, Verdolini K, Hebda PA (June 2005). "Biochemical markers associated with acute vocal fold wound healing: a rabbit model". J Voice. 19 (2): 283–9. doi:10.1016/j.jvoice.2004.04.003. PMID 15907442. 
  44. ^ Hansen JK, Thibeault SL (March 2006). "Current understanding and review of the literature: vocal fold scarring". J Voice. 20 (1): 110–20. doi:10.1016/j.jvoice.2004.12.005. PMID 15964741. 
  45. ^ Ferrein, Antoine (1741). "De la formation de la voix de l'homme". Mémoires de l' Académie Royale (in French). Paris: Bondot: 409–432. 
  46. ^ Wilson, Kenneth G. (1993). The Columbia Guide to Standard American English. Archived from the original on 2008-01-13. 
  47. ^ Zimmer, Ben (2007-10-18). "Are We Giving Free Rei(g)n to New Spellings?". OUPblog. Oxford University Press. Archived from the original on 2009-01-31. Retrieved 2008-11-13. 
  48. ^ "National Dictionary Day". ABC News. 2007-10-16. Retrieved 2008-11-13. [dead link]
  49. ^ Catford, J. C. (1988). A Practical Introduction to Phonetics. Oxford University Press. pp. 9, 22, 37. ISBN 0-19-824217-4. 
  50. ^ Ladefoged, Peter; Disner, Sandra Ferrari (2012). Vowels and Consonants (3rd ed.). Wiley-Blackwell. p. 20. ISBN 978-1-4443-3429-6. 
  51. ^ Reetz, Henning; Jongman, Allard (2009). Phonetics: Transcription, Production, Acoustics, and Perception. Wiley-Blackwell. p. 72. ISBN 978-0-631-23225-4. 

External links[edit]

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