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Sperm motility

Sperm motility describes the ability of sperm to move properly through the female reproductive tract (internal fertilization) or through water (external fertilization) to reach the egg. Sperm motility can also be thought of as the quality, which is a factor in successful conception; sperm that do not "swim" properly will not reach the egg in order to fertilize it. Sperm motility in mammals also facilitates the passage of the sperm through the cumulus oophorus (a layer of cells) and the zona pellucida (a layer of extracellular matrix), which surround the mammalian oocyte.

Video of human sperm cells moving under a microscope

In the wood mouse Apodemus sylvaticus, sperms aggregate in 'trains' that are better able to fertilize eggs because they are more capable of navigating the viscous environment of the female reproductive tract. The trains move in a sinusoidal motion.

Sperm motility is also affected by certain factors released by eggs.[1]

Sperm movement is activated by changes in intracellular ion concentration.[2] The changes in ion concentration that provoke motility are different among species. In marine invertebrates and sea urchins, the rise in pH to about 7.2–7.6 activates ATPase which leads to a decrease in intracellular potassium, and thus induces membrane hyperpolarization. As a result, sperm movement is activated.[3] The change in cell volume which alters intracellular ion concentration can also contribute to the activation of sperm motility. In some mammals, sperm motility is activated by increase in pH, calcium ion and cAMP, yet it is suppressed by low pH in the epididymis.

The tail of the sperm - the flagellum - confers motility upon the sperm, and has three principal components:

  1. a central skeleton constructed of 11 microtubules collectively termed the axoneme and similar to the equivalent structure found in cilia
  2. a thin cell membrane covering the axoneme
  3. mitochondria arranged spirally around the axoneme at the middle-piece,

Back and forth movement of the tail results from a rhythmical longitudinal sliding motion between the anterior and posterior tubules that make up the axoneme. The energy for this process is supplied by ATP produced by mitochondria. The velocity of a sperm in fluid medium is usually 1–4 mm/min. This allows the sperm to move towards an ovum in order to fertilize it.

The axoneme is attached at its base to a centriole known as the distal centriole and acts as a basal body.[4] In most animals, this distal centriole act as a shock absorber preventing the microtubules filaments from moving at the axoneme base. In contrast, in mammals, the distal centriole evolved an atypical structure, known as the atypical distal centriole.[5] The atypical centriole is made of splayed microtubules organized into left and right sides. During sperm movement, the two sides move relative to each other, helping to shape the waveform of the sperm tail.[5]

In mammals, spermatozoa mature functionally through a process which is known as capacitation. When spermatozoa reach the isthmic oviduct, their motility has been reported to be reduced as they attach to epithelium. Near the time of ovulation, hyperactivation occurs. During this process, the flagella move with high curvature and long wavelength.[6] Hyperactivation is initiated by extracellular calcium; however, the factors that regulate calcium level is unknown.[7]

Without technological intervention, a non-motile or abnormally-motile sperm is not going to fertilize. Therefore, the fraction of a sperm population that is motile is widely used as a measure of semen quality . Insufficient sperm motility is a common cause of subfertility or infertility. Several measures are available to improve sperm quality.

Axoneme movement edit

Sperm motility is dependent on several metabolic pathways and regulatory mechanisms.

The axonemal bend movement is based on the active sliding of axonemal doublet microtubules by the molecular motor dynein, which is divided into an outer and an inner arm. Outer and inner arm plays different roles in the production and regulation of flagellar motility: the outer arm increase the beat frequency, the inner arm is involved in the propulsion and propagation of flagellar bending. The bending of the flagellum is due to subsequent cycles of dynein arm attachment, generation of force and detachment on the B subunit. The binding of the axoneme is the result of the presence of a resistance to the microtubule sliding generated by dynein.

Dyneins on the two sides of the central pair apparatus are regulated in an opposite way by an activation/disactivation game made by the radialspoke-central pair apparatus, that regulates the flagellar bending. Sperm motility is regulated by several pathways and the most important are the Calcium pathway and the PKA pathway. This pathwaysinvolve ions, adenylyl cyclase, cAMP, membrane channels and phosphorylations.

The first event is the activation of a Na+/HCO3 (NBC) co-transporter and the regulation of HCO3 /Cl by SLC26 transporters, that bring to an increase in HCO3 levels.

The second event is the activation of an Na+/H+ exchanger and of the proton channel Hv-1, that leads to an increase in pH levels.

These increase in HCO3 and pH levels bring to the activation of the CatSper channel, a sperm membrane specific calcium channel. CatSperm can be activated also by progesterone and albumine. CatSper, once activated, opens and let free calcium entrance inside the cell, with a global increase in calcium intracellular levels.

Together, the increase in HCO3 , pH and calcium leads to the activation of a soluble adenylyl cyclase (SAC or SACY), that increases the production of cAMP and brings to the activation of PKA, a protein kinase that phosphorylates several tyrosine kinases and leads to a phosphorylation cascade that ends with the phosphorylation of the axonemal dynein and the start of flagellar movement.[8]

Sperm DNA damage edit

Sperm DNA damage is common in infertile men.[9] About 31% of men with sperm motility defects have high levels of sperm DNA fragmentation.[10]

Sperm Motility and Age edit

Sperm motility increases from puberty through one's mid-thirties. Research shows that from the age of 36 onwards, sperm motility decreases from 40% Grade A & B to 31% in one's 50s. The effects of aging on semen quality is summarized below based on a study of 1,219 subjects:[11]

Age group (years) Number of subjects (n) Motility (% Grade A+B)

[Min-Max]

21-28 57 47.5 ± 25.4

[0-88]

29-35 450 48.1 ± 30.4

[0-95]

36-42 532 40.0 ± 27.1

[0-83]

43-49 165 33.1 ± 25.1

[0-84]

50-60 15 31.3 ± 23.9

[0-59]

Classifications of motility edit

  1. Straight moving,
  2. Zig-zag moving,
  3. Vibrating,
  4. Non-motile

References edit

  1. ^ Quill, A. T., Garbers, L. D. (2002). "Sperm Motility Activation and Chemoattraction". In Daniel M. Hardy (ed.). Fertilization. California: Academic press. p. 29. ISBN 978-0-12-311629-1.{{cite book}}: CS1 maint: multiple names: authors list (link)
  2. ^ Jensen, Martin Blomberg (March 2014). "Vitamin D and male reproduction". Nature Reviews Endocrinology. 10 (3): 175–186. doi:10.1038/nrendo.2013.262. PMID 24419359. S2CID 32394600.
  3. ^ Darszon, Alberto; Labarca, Pedro; Nishigaki, Takuya; Espinosa, Felipe (1 April 1999). "Ion Channels in Sperm Physiology". Physiological Reviews. 79 (2): 481–510. doi:10.1152/physrev.1999.79.2.481. PMID 10221988. S2CID 30768971.
  4. ^ Avidor-Reiss, Tomer; Carr, Alexa; Fishman, Emily Lillian (December 2020). "The sperm centrioles". Molecular and Cellular Endocrinology. 518: 110987. doi:10.1016/j.mce.2020.110987. PMC 7606549. PMID 32810575.
  5. ^ a b Fishman, Emily L.; Jo, Kyoung; Nguyen, Quynh P. H.; Kong, Dong; Royfman, Rachel; Cekic, Anthony R.; Khanal, Sushil; Miller, Ann L.; Simerly, Calvin; Schatten, Gerald; Loncarek, Jadranka; Mennella, Vito; Avidor-Reiss, Tomer (December 2018). "A novel atypical sperm centriole is functional during human fertilization". Nature Communications. 9 (1): 2210. Bibcode:2018NatCo...9.2210F. doi:10.1038/s41467-018-04678-8. PMC 5992222. PMID 29880810.
  6. ^ Mortimer, D; Aitken, Rj; Mortimer, St; Pacey, Aa (1995). "Workshop report: clinical CASA--the quest for consensus". Reproduction, Fertility and Development. 7 (4): 951–959. doi:10.1071/RD9950951. PMID 8711226.
  7. ^ Yanagimachi, R. (1994). "Mammalian fertilization". In Knobil, E.; Neill, J. D. (eds.). The Physiology of Reproduction. New York: Raven Press. pp. 189–317.[ISBN missing]
  8. ^ Sun, Xiang-hong; Zhu, Ying-ying; Wang, Lin; Liu, Hong-ling; Ling, Yong; Li, Zong-li; Sun, Li-bo (December 2017). "The Catsper channel and its roles in male fertility: a systematic review". Reproductive Biology and Endocrinology. 15 (1): 65. doi:10.1186/s12958-017-0281-2. PMC 5558725. PMID 28810916.
  9. ^ Simon, Luke; Lutton, Deborah; McManus, Joanne; Lewis, Sheena E.M. (February 2011). "Sperm DNA damage measured by the alkaline Comet assay as an independent predictor of male infertility and in vitro fertilization success". Fertility and Sterility. 95 (2): 652–657. doi:10.1016/j.fertnstert.2010.08.019. PMID 20864101.
  10. ^ Belloc, Stephanie; Benkhalifa, Moncef; Cohen-Bacrie, Martine; Dalleac, Alain; Chahine, Hikmat; Amar, Edouard; Zini, Armand (May 2014). "Which isolated sperm abnormality is most related to sperm DNA damage in men presenting for infertility evaluation". Journal of Assisted Reproduction and Genetics. 31 (5): 527–532. doi:10.1007/s10815-014-0194-3. PMC 4016368. PMID 24566945.
  11. ^ Kumar, M.D., Naina; Singh, M.D., Amit K; Choudhari, M.D., Ajay R (August 2017). "Impact of age on semen parameters in male partners of infertile couples in a rural tertiary care center of central India: A cross-sectional study". International Journal of Reprodroductive Biomedicine. 15 (8): 497–502.

External links edit

  • Sperm motility, Colorado State University
  • Semen analysis - how to interpret a semen analysis report, Malpani Infertility Clinic
  • Sperm count analysis

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Sperm motility describes the ability of sperm to move properly through the female reproductive tract internal fertilization or through water external fertilization to reach the egg Sperm motility can also be thought of as the quality which is a factor in successful conception sperm that do not swim properly will not reach the egg in order to fertilize it Sperm motility in mammals also facilitates the passage of the sperm through the cumulus oophorus a layer of cells and the zona pellucida a layer of extracellular matrix which surround the mammalian oocyte source source source source source source Video of human sperm cells moving under a microscopeIn the wood mouse Apodemus sylvaticus sperms aggregate in trains that are better able to fertilize eggs because they are more capable of navigating the viscous environment of the female reproductive tract The trains move in a sinusoidal motion Sperm motility is also affected by certain factors released by eggs 1 Sperm movement is activated by changes in intracellular ion concentration 2 The changes in ion concentration that provoke motility are different among species In marine invertebrates and sea urchins the rise in pH to about 7 2 7 6 activates ATPase which leads to a decrease in intracellular potassium and thus induces membrane hyperpolarization As a result sperm movement is activated 3 The change in cell volume which alters intracellular ion concentration can also contribute to the activation of sperm motility In some mammals sperm motility is activated by increase in pH calcium ion and cAMP yet it is suppressed by low pH in the epididymis The tail of the sperm the flagellum confers motility upon the sperm and has three principal components a central skeleton constructed of 11 microtubules collectively termed the axoneme and similar to the equivalent structure found in cilia a thin cell membrane covering the axoneme mitochondria arranged spirally around the axoneme at the middle piece Back and forth movement of the tail results from a rhythmical longitudinal sliding motion between the anterior and posterior tubules that make up the axoneme The energy for this process is supplied by ATP produced by mitochondria The velocity of a sperm in fluid medium is usually 1 4 mm min This allows the sperm to move towards an ovum in order to fertilize it The axoneme is attached at its base to a centriole known as the distal centriole and acts as a basal body 4 In most animals this distal centriole act as a shock absorber preventing the microtubules filaments from moving at the axoneme base In contrast in mammals the distal centriole evolved an atypical structure known as the atypical distal centriole 5 The atypical centriole is made of splayed microtubules organized into left and right sides During sperm movement the two sides move relative to each other helping to shape the waveform of the sperm tail 5 In mammals spermatozoa mature functionally through a process which is known as capacitation When spermatozoa reach the isthmic oviduct their motility has been reported to be reduced as they attach to epithelium Near the time of ovulation hyperactivation occurs During this process the flagella move with high curvature and long wavelength 6 Hyperactivation is initiated by extracellular calcium however the factors that regulate calcium level is unknown 7 Without technological intervention a non motile or abnormally motile sperm is not going to fertilize Therefore the fraction of a sperm population that is motile is widely used as a measure of semen quality Insufficient sperm motility is a common cause of subfertility or infertility Several measures are available to improve sperm quality Contents 1 Axoneme movement 2 Sperm DNA damage 3 Sperm Motility and Age 4 Classifications of motility 5 References 6 External linksAxoneme movement editSperm motility is dependent on several metabolic pathways and regulatory mechanisms The axonemal bend movement is based on the active sliding of axonemal doublet microtubules by the molecular motor dynein which is divided into an outer and an inner arm Outer and inner arm plays different roles in the production and regulation of flagellar motility the outer arm increase the beat frequency the inner arm is involved in the propulsion and propagation of flagellar bending The bending of the flagellum is due to subsequent cycles of dynein arm attachment generation of force and detachment on the B subunit The binding of the axoneme is the result of the presence of a resistance to the microtubule sliding generated by dynein Dyneins on the two sides of the central pair apparatus are regulated in an opposite way by an activation disactivation game made by the radialspoke central pair apparatus that regulates the flagellar bending Sperm motility is regulated by several pathways and the most important are the Calcium pathway and the PKA pathway This pathwaysinvolve ions adenylyl cyclase cAMP membrane channels and phosphorylations The first event is the activation of a Na HCO3 NBC co transporter and the regulation of HCO3 Cl by SLC26 transporters that bring to an increase in HCO3 levels The second event is the activation of an Na H exchanger and of the proton channel Hv 1 that leads to an increase in pH levels These increase in HCO3 and pH levels bring to the activation of the CatSper channel a sperm membrane specific calcium channel CatSperm can be activated also by progesterone and albumine CatSper once activated opens and let free calcium entrance inside the cell with a global increase in calcium intracellular levels Together the increase in HCO3 pH and calcium leads to the activation of a soluble adenylyl cyclase SAC or SACY that increases the production of cAMP and brings to the activation of PKA a protein kinase that phosphorylates several tyrosine kinases and leads to a phosphorylation cascade that ends with the phosphorylation of the axonemal dynein and the start of flagellar movement 8 Sperm DNA damage editSperm DNA damage is common in infertile men 9 About 31 of men with sperm motility defects have high levels of sperm DNA fragmentation 10 Sperm Motility and Age editSperm motility increases from puberty through one s mid thirties Research shows that from the age of 36 onwards sperm motility decreases from 40 Grade A amp B to 31 in one s 50s The effects of aging on semen quality is summarized below based on a study of 1 219 subjects 11 Age group years Number of subjects n Motility Grade A B Min Max 21 28 57 47 5 25 4 0 88 29 35 450 48 1 30 4 0 95 36 42 532 40 0 27 1 0 83 43 49 165 33 1 25 1 0 84 50 60 15 31 3 23 9 0 59 Classifications of motility editStraight moving Zig zag moving Vibrating Non motileReferences edit Quill A T Garbers L D 2002 Sperm Motility Activation and Chemoattraction In Daniel M Hardy ed Fertilization California Academic press p 29 ISBN 978 0 12 311629 1 a href Template Cite book html title Template Cite book cite book a CS1 maint multiple names authors list link Jensen Martin Blomberg March 2014 Vitamin D and male reproduction Nature Reviews Endocrinology 10 3 175 186 doi 10 1038 nrendo 2013 262 PMID 24419359 S2CID 32394600 Darszon Alberto Labarca Pedro Nishigaki Takuya Espinosa Felipe 1 April 1999 Ion Channels in Sperm Physiology Physiological Reviews 79 2 481 510 doi 10 1152 physrev 1999 79 2 481 PMID 10221988 S2CID 30768971 Avidor Reiss Tomer Carr Alexa Fishman Emily Lillian December 2020 The sperm centrioles Molecular and Cellular Endocrinology 518 110987 doi 10 1016 j mce 2020 110987 PMC 7606549 PMID 32810575 a b Fishman Emily L Jo Kyoung Nguyen Quynh P H Kong Dong Royfman Rachel Cekic Anthony R Khanal Sushil Miller Ann L Simerly Calvin Schatten Gerald Loncarek Jadranka Mennella Vito Avidor Reiss Tomer December 2018 A novel atypical sperm centriole is functional during human fertilization Nature Communications 9 1 2210 Bibcode 2018NatCo 9 2210F doi 10 1038 s41467 018 04678 8 PMC 5992222 PMID 29880810 Mortimer D Aitken Rj Mortimer St Pacey Aa 1995 Workshop report clinical CASA the quest for consensus Reproduction Fertility and Development 7 4 951 959 doi 10 1071 RD9950951 PMID 8711226 Yanagimachi R 1994 Mammalian fertilization In Knobil E Neill J D eds The Physiology of Reproduction New York Raven Press pp 189 317 ISBN missing Sun Xiang hong Zhu Ying ying Wang Lin Liu Hong ling Ling Yong Li Zong li Sun Li bo December 2017 The Catsper channel and its roles in male fertility a systematic review Reproductive Biology and Endocrinology 15 1 65 doi 10 1186 s12958 017 0281 2 PMC 5558725 PMID 28810916 Simon Luke Lutton Deborah McManus Joanne Lewis Sheena E M February 2011 Sperm DNA damage measured by the alkaline Comet assay as an independent predictor of male infertility and in vitro fertilization success Fertility and Sterility 95 2 652 657 doi 10 1016 j fertnstert 2010 08 019 PMID 20864101 Belloc Stephanie Benkhalifa Moncef Cohen Bacrie Martine Dalleac Alain Chahine Hikmat Amar Edouard Zini Armand May 2014 Which isolated sperm abnormality is most related to sperm DNA damage in men presenting for infertility evaluation Journal of Assisted Reproduction and Genetics 31 5 527 532 doi 10 1007 s10815 014 0194 3 PMC 4016368 PMID 24566945 Kumar M D Naina Singh M D Amit K Choudhari M D Ajay R August 2017 Impact of age on semen parameters in male partners of infertile couples in a rural tertiary care center of central India A cross sectional study International Journal of Reprodroductive Biomedicine 15 8 497 502 External links edit nbsp Wikimedia Commons has media related to Sperm motility Sperm motility Colorado State University Semen analysis how to interpret a semen analysis report Malpani Infertility Clinic Sperm count analysis Retrieved from https en wikipedia org w index php title Sperm motility amp oldid 1190876362, wikipedia, wiki, book, books, library,

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