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II. Neurological Neuroanatomy

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Title: II. Neurological Neuroanatomy


1
II. Neurological Neuroanatomy
  • Lecture 2

2
Neurological Histology
  • Histology is the microscopic study of the
    structure of tissues.
  • In the nervous system, the two broad classes of
    cells are neurons and glia.
  • Within each class there are many different types
    of cells that differ based on their structure,
    chemistry, and function.

3
Classes of Cells
  • Neurons are the most important cells of the
    unique functions of the brain.
  • They sense changes in the environment,
    communicate these changes to other neurons, and
    command the bodys responses to these sensations.

4
Classes of Cells
  • Glia are thought to contribute to brain function
    mainly by insulating, supporting, and nourishing
    neighboring neurons.
  • In fact, the term glia is derived from the Greek
    word for glue, giving the impression that the
    main function of these cells is to keep the brain
    from running out of our ears.

5
Analogy Cookie and Brain
  • If your brain were a chocolate-chip cookie and
    the neurons the chocolate chips, the glia would
    be the cookie dough that fill all the other
    spaces and ensures that the chips are suspended
    in their appropriate locations.

6
Brainstem Structure and Function
  • We are going to spend a bit of time looking more
    thoroughly at the structure and function of the
    brainstem.
  • In particular, we will focus on cranial nerves
    and their nuclei, ascending and descending
    tracts, specific nuclei of the reticular
    formation, and other select special nuclei.

7
Cranial Nerves
  • Cranial nerves (CN) I Olfactory and II Optic are
    part of the forebrain.
  • The other 10 cranial nerves originate in the
    brainstem.
  • Some cranial nerves serve only sensory functions
    other serve only motor functions.
  • Many of the nerves are mixed, serving both
    sensory and motor functions.

8
Cranial Nerves
  • The three main functions of the cranial nerves
    are as follows
  • Motor and sensory innervation of the head and
    neck
  • Innervation of special sense organs
  • Innervation of the parasympathetic autonomic
    ganglia that control important visceral
    functions such as breathing, heart rate, blood
    pressure, coughing, and swallowing.

9
Cranial Nerves
  • An assessment of the functioning of the cranial
    nerves is an extremely important part of a
    clinical neurological examination.
  • Disease states in the brain are often reflected
    in functional abnormalities of one or more of the
    cranial nerves.

10
Cranial Nerves
  • Since the cranial nerves originate from different
    regions in the brainstem, disorder in the
    function of one or more nerves can provide
    valuable information about the site of lesion.

11
Ventrally Located Cranial Nerves
  • Cranial nerves III, VI, and XII are seen exiting
    from the ventral side of the brainstem, close to
    the midline.

12
Ventrally Located Cranial Nerves
  • The oculomotor nerve (III) emerges at the caudal
    border of the midbrain.
  • It innervates the extraocular muscles

13
Ventrally Located Cranial Nerves
  • The abducens nerve (VI) emerges at the caudal
    border of the pons.
  • It also innervates the extraocular muscles

14
Ventrally Located Cranial Nerves
  • The hypoglossal nerve (XII) emerges from the
    medulla just lateral to the medullary pyramids.
  • It innervates the intrinsic muscles of the tongue

15
Dorsally Located Cranial Nerve
  • Only one cranial nerve, the trochlear nerve (IV)
    exits from the dorsal aspect of the brainstem.
  • The trochlear nerve exits from the midbrain just
    below the inferior colliculus near the midline to
    innervate the superior oblique muscle of the eye.

16
Laterally Located Cranial Nerves
  • The 8 remaining cranial nerves exit laterally
    from the brainstem.
  • The trigeminal nerve (V) exits the pons.
  • It mediates sensation from facial skin and
    innervates the muscles of mastication.

17
Laterally Located Cranial Nerves
  • The facial (VII) and the vestibulocochlear (VIII)
    nerves originate at the junction between the pons
    and medulla.

18
Laterally Located Cranial Nerves
  • The glossopharyngeal (IX), vagus (X), and
    accessory (XI) nerves arise in the medulla as a
    series of fine rootlets just dorsal to the
    inferior olive.

19
Functional Classification of CNs
  • Cranial nerves serve general motor and general
    sensory functions as well as special functions
    resulting from the use of special receptors and
    neurons.
  • The general and special function of CNs can be
    further classified by
  • whether the nerve innervates somatic muscles or
    visceral structures
  • Whether it is involved in sensory (afferent) or
    motor (efferent) information.

20
Functional Components of NS
21
Functional Components of NS
22
Cranial Nerve Nuclei
  • As in the spinal cord, the cell bodies of motor
    and sensory neurons differ in location from one
    another.
  • The cell bodies of motor neurons that send their
    axons into the cranial nerves are located within
    the brainstem.
  • The cell bodies of the afferent fibers in the
    cranial nerves lie outside the brainstem, either
    in ganglia or in specialized end-organs such as
    the eye.

23
Cranial Motor Nuclei
  • The cranial motor nuclei of all general somatic,
    general visceral, and special somatic motor
    neurons (shown in red) are located in the
    brainstem.
  • These cranial motor neurons are called lower
    motor neurons.

24
Cranial Nuclei Organization
  • Cranial nerve nuclei are organized into seven
    longitudinal columns rostrocaudally in the
    brainstem according to function.

25
Somatic Efferent Column
  • CN nuclei III, IV, VI, and XII that innervate
    somatic muscles in the head derived from myotomes
    are situated close to the midline and immediately
    ventral to the floor of the fourth ventricle
    (red).

26
Special Visceral Efferent Column
  • CN nuclei V, VII, IX, X, and XI that innervate
    the branchiomeric muscles are displaced ventrally
    and laterally from the somatic motor column
    (orange).
  • The cell bodies of CNs IX and X are clustered in
    a single group called the nucleus ambiguus.

27
Nucleus Ambiguus
  • The nucleus ambiguus is so named because it is
    penetrated by fibers running from the inferior
    olive to the cerebellum and is consequently
    difficult to identify in sections stained for
    cell bodies.
  • Neurons in the nucleus ambiguus innervate
    striated muscles in the larynx and pharynx and
    are critical for speech and swallowing.

28
General Visceral Efferent Column
  • The parasympathetic neurons of CNs III, VII, IX,
    X are found immediately lateral to the somatic
    motor column (yellow).
  • They regulate specific autonomic functions.

29
GVE Column Functions
  • The oculomotor cranial nerve (III) innervates the
    smooth muscle of the eyelid, the pupillary
    constrictor, and Muellers muscle, which holds
    the eye forward in the orbit.
  • Damage to this autonomic component of the CN III
    results in eyelid droop (ptosis), pupil dilation
    (mydriasis) and the eye being drawn forward in
    the orbit (exophthalmos).

30
GVE Column Functions
  • The superior salivatory and inferior salivary
    nuclei are another group of general visceral
    column motor nuclei.
  • The axons from the superior salivatory nucleus
    run in the root of the facial nerve (VII).
  • The axons from the inferior salivary nucleus run
    in the glossopharyngeal (IX) nerve.
  • Together they innervate various salivary and
    mucous glands.

31
GVE Column Functions
  • Finally, the dorsal motor nucleus of the vagus
    (X) CN innervates the viscera of the body the
    heart, the lungs, and the gut.
  • In the gut, the CN X promotes peristalsis.

32
Cranial Sensory Nuclei
  • The cell bodies of the afferent fibers supplying
    the cranial nerves lie outside the brainstem.
  • The sensory nuclei in the brainstem are composed
    of second order neurons that receive input from
    the primary sensory neurons.

33
General Visceral Afferent Column
  • Second order neuronal cell bodies of the general
    visceral afferent column (blue check) lie
    adjacent to the general visceral efferent column.

34
General Visceral Afferent Column
  • They receive fibers conveying the sense of taste,
    as well as those carrying input from the larynx
    and pharynx, and the heart, lungs, and gut.
  • In the medulla, this column of cells is called
    the nucleus tractus solitarius (NTS).

35
Nucleus Tractus Solitarius
  • The neurons conveying sensory input to the NTS
    have their cell bodies in ganglia that lie
    outside the brainstem in association with cranial
    nerves VII (facial), IX (glossopharyngeal), and X
    (vagus).
  • The axons from these ganglia run into the
    brainstem and join the solitary tract which
    terminate in the NTS.

36
Nucleus Tractus Solitarius
  • The rostral end of the NTS is the relay for taste
    sensation.
  • Axons from these nuclei synapse in the thalamus.
  • From the thalamic nuclei, information about taste
    is relayed to the cerebral cortex.

37
Nucleus Tractus Solitarius
  • The other regions of the nucleus deal with
    cardiovascular functions.
  • They have local connections with the reticular
    formation, and indirect connections with the
    limbic system in regulating autonomic tone.

38
Special Somatic Afferent Column
  • The SSA column (purple dots) lies lateral to the
    general visceral afferent column.
  • The SSA nuclei in the caudal part of the pons and
    the rostral part of the medulla receive fibers of
    the vestibulocochlear nerve (VIII).

39
Special Somatic Afferent Column
  • The cochlear nuclei (CN) receive input from the
    cochlear division of CN VIII.
  • The vestibular nuclei (VN) receive input from the
    visceral division of CN VIII.

40
General Somatic Afferent Column
  • The general somatic afferent column is displaced
    ventrolaterally (green dots).
  • It is composed of the three separate divisions of
    the sensory trigeminal nucleus (V).

41
General Somatic Afferent Column
  • The portion of the nucleus which lies in the
    midbrain modulates proprioception from the
    muscles and joints of the face.

42
General Somatic Afferent Column
  • The main sensory nucleus lies in the pons.
  • The portion of the nucleus which lies in the
    medulla receives input from the muscles, skin,
    joints of the face, and mucous membranes of the
    mouth.

43
Cranial Nerve Organization
  • Three principles underlie the organization of the
    cranial nerves.
  • First, most of the motor nuclei associated in the
    brainstem are associated with individual cranial
    nerves.

44
Cranial Nerve Organization
  • For example, the trigeminal nerve has it own
    motor nucleus.
  • They receive input from motor areas of the
    cerebral cortex and send their axons to muscles
    in the periphery.

45
Cranial Nerve Organization
  • Second, afferent nuclei in the brainstem often
    receive fibers from several cranial nerves.
  • The NTS, for example, collects fibers carrying
    information about taste from the facial (VII),
    glossopharyngeal (IX), and vagus (X) nerves.

46
Cranial Nerve Organization
  • The medullary nucleus of the trigeminal nerve
    also receives sensory input from several cranial
    nerves.
  • The interesting point is that sensory information
    of a particular type, such as taste, is forwarded
    to a single nucleus, no matter which cranial
    nerve pathway it takes.

47
Cranial Nerve Organization
  • The third principle is related to location
    neurons with different functional properties
    occupy consistently different positions in the
    brainstem.
  • This specificity of localization arises during
    development.

48
Cranial Nerve Organization
  • Neurons destined for different functions arise
    from distinctive parts of the neuroepithelial
    lining of the neural tube.

49
Cranial Nerve Organization
  • They differentiate at characteristic times in
    development, and migrate to specific positions in
    the brainstem.

50
Communicative Pathways
  • There are four major communicative pathways
    through the brainstem.
  • The corticospinal and the corticobulbar tracts
    constitute the motor pathways.
  • The medial lemniscal and the spinothalamic tracts
    constitute the sensory pathways.

51
Corticospinal Tract
  • The corticospinal tract descends in the ventral
    aspect of the brainstem within the pyramids to
    the caudal border of the medulla where it crosses
    to form the lateral corticospinal tract.

52
Corticobulbar Tract
  • Corticobulbar fibers also run in the pyramids,
    but they peel off at various levels to reach the
    motor nuclei of the cranial nerves.

53
Corticobulbar Tract
  • The neurons that give rise to corticobulbar axons
    are upper motor neurons whose effects are similar
    to those exerted by the corticospinal axons upon
    spinal motor neurons.

54
Medial Lemniscal Pathway
  • The medial lemniscal pathway is the brainstem
    pathway component of the dorsal column nuclei
    (fasciculi cuneatus and gracilis)

55
Medial Lemniscal Pathway
  • The axons of the medial lemniscus pathway (blue)
    ascend initially near midline and move out
    laterally in the lemniscus as they approach the
    thalamus.

56
Spinothalamic Tract
  • The spinothalamic tract (red) runs near the
    medial lemniscus after ascending from its origin
    in the spinal cord.

57
Reticular Neurons and Processes
  • Aside from these tracts and a few others, the
    major cranial nerve nuclei, and nuclei related to
    cerebellar function, the rest of the brainstem is
    composed of reticular neurons and their
    processes.
  • These neurons and processes found outside the
    major nuclear groups of the brainstem constitute
    the reticular formation.

58
Reticular Formation
  • As an entity, the reticular formation represents
    an extensive elaboration of the rostral portion
    of the interneuronal network found in the spinal
    cord.
  • It is distributed throughout the medulla, pons,
    and midbrain.

59
Reticular Neurons
  • Lying in the midline are the raphe nuclei, so
    named because of their proximity to the midline
    seam or raphe.

60
Reticular Neurons
  • Adjacent to the raphe is the large-cell region of
    the reticular formation and more laterally still
    is the small-group region.

61
Reticular Axons
  • Nearly all reticular neurons have far-flung
    distribution of their axons in both caudal and
    rostral directions along the brainstem.
  • Overlapping afferents, of which some are
    inhibitory and others facilitatory, converge on a
    given reticular neuron.

62
Reticular Afferents
  • Reticular afferents consist of all collaterals
    from the ascending and descending spinal tracts
    (pain, proprioception, tactile, temperature,
    vibration), cranial nerve nuclei, cerebellum,
    midbrain, thalamus, subthalamus, hypothalamus,
    striatum, limbic lobe, and various cortical areas.

63
Reticular Nuclei
  • Reticular nuclei also send input to brain
    structures such as the cochlear and vestibular
    nuclei, tectal (colliculi), and pretectal
    structures (red nucleus), geniculate nuclei, and
    thalamic nuclei that process specialized and
    general sensory input.

64
Reticular Influences
  • Through its direct and indirect projections, the
    reticular formation influences all nervous system
    functions.
  • It sends projections to somatic and autonomic
    nuclei in general.
  • Reticular afferents also project to autonomic and
    somatic motor nuclei of cranial nerves in the
    brainstem, and they relay information to
    interneuronal pools in the spinal cord.

65
Reticular Influences
  • There also project directly and indirectly to the
    cerebellum, red nucleus, substantia nigra,
    midbrain tectum, subthalamic nuclei,
    hypothalamus, thalamus, and limbic lobe (septum,
    hippocampus, amygdala, and cingulate gyrus).

66
Reticular Influences
  • Direct reticular projections influence
    information processing by either accentuating or
    attenuating the sensory (audition, vision,
    olfaction, pain, temperature, and tactile)
    stimuli.
  • For example, reticulospinal projections modulate
    the quantity and quality of sensory information.

67
Reticular Influences
  • They employ gating mechanisms at both pre- and
    post-synaptic terminals to affect sensory impulse
    transmission at both spinal and thalamic levels.
  • Within the reticular formation, specific nuclear
    cell aggregates form closed-loop circuits and
    serve as the reticular centers for regulating
    various sensorimotor, visceral, and cortical
    activating functions.

68
Reticular Influences
  • For example, most coma-causing lesions are found
    at the midbrain, hypothalamic, and thalamic
    junctions.
  • Impairment at the level of the midbrain reticular
    formation has been implicated.
  • Reticular centers may combine to form reticular
    networks that regulate complex sensorimotor and
    visceral behaviors, such as eating, swallowing,
    vomiting, coughing, sneezing, copulation, and
    fighting.

69
Reticular Influences
  • Integrated motor functions include activities
    that are vital to survival and are controlled by
    brainstem reticular nuclei.
  • Convergent multimodal input and diffuse divergent
    output regulate cardiac activity, respiration,
    and swallowing.

70
Vasomotor Functions
  • The reticular nuclei regulating vasomotor
    functions of the heart extend from the rostral
    medulla to the mid pons.
  • These nuclei receive extensive projections from
    peripheral receptors and are in part controlled
    by the hypothalamus.
  • They project information via fibers of the vagus
    nerve.

71
Vasomotor Functions
  • Stimulation of the lateral reticular pressor
    center in the upper medulla increases heart rate
    and causes vasoconstriction.
  • Stimulation of the lateral reticular depressor
    center in the lower medulla decreases heart rate
    and causes vasodilation.

72
Vasomotor Functions
  • Lesions of the medullary cardiovascular center
    can cause cardiac irregularities and blood
    pressure changes, both of which are
    life-threatening.

73
Respiratory Functions
  • The automatic brainstem respiratory center
    consists of several groups of scattered neurons
    in the reticular formation.
  • It can be divided into two distinct centers
    pontine centers and medullary respiratory center.

74
Respiratory Functions
  • The medullary respiratory group consists of the
    dorsal respiratory group and the ventral
    respiratory group of neurons.

75
Respiratory Functions
  • The dorsal medullary respiratory center contains
    reticular nuclei which are responsive to
    afferents from the carotid and aortic
    chemoreceptors through the vagus and
    glossopharyngeal nerves.
  • These signals, along with sensory information
    from the lungs, help control respiratory activity.

76
Respiratory Functions
  • The fibers descending from the dorsal medullary
    respiratory neurons cross to activitate spinal
    cord nerves to cause contraction of the diaphragm
    to begin the cycle of inspiration.

77
Respiratory Functions
  • The ventral group of respiratory nuclei are
    inactive during the normal respiratory cycle.
  • It is activated when high levels of pulmonary
    ventilation are required.

78
Respiratory Function
  • Projections from the ventral medullary
    respiratory nuclei cross to activate the needed
    thoracic muscles.
  • Both the dorsal and ventral respiratory nuclei of
    the medulla contain the mechanism responsible for
    controlling the rhythmic activity of the
    respiratory muscles.

79
Respiratory Function
  • The pontine respiratory centers generally control
    the duration, depth, and rate of the respiratory
    cycle.
  • Because exhalation is normally passive, the
    pneumotaxic area seeks to limit the duration of
    inspiratory phase of the lungs by constant
    inhibition of the medullary respiratory centers.

80
Respiratory Function
  • A lesion in the ponto-medullary respiratory
    center causes asphyxia and eventually death if
    artificial respiration is not administered.
  • As with respiration, the reticular formation
    regulate the acts of swallowing, vomiting, and
    coughing, by integrating the function of several
    nerve pathways.

81
Swallowing Function
  • For swallowing, the reticular formation
    integrates functions of cranial nerves V, VII,
    IX, X, and XII.
  • Specifically, the reticular swallowing center
    directs projections to the adjacent respiratory
    center and to the nuclei of V, VII, IX, X, and
    XII, to initiate a series of fixed action motor
    patterns that ensure proper breathing management
    while the bolus passes through the pharynx.

82
Swallowing Function
  • As the bolus passes out of the pharynx, the
    reticular respiratory center regulates the
    reopening of the respiratory passageway.
  • Brainstem lesions interrupting afferent and
    efferent projections of the reticular formation
    can alter the integrity of the swallow response.

83
Vomiting Function
  • Vomiting is regulated in the medullary reticular
    formation where it receives input from the
    oropharynx and gastrointestinal tract.
  • Noxious impulses mediating irritations of the
    intestinal tract and oropharynx initiate
    reflexive vomiting.

84
Vomiting Function
  • Projections from the vomiting center in the
    medulla descend through the fibers of cranial
    nerves X and IX and coordinate the contraction of
    the abdominal, diaphragmatic, and intercostal
    muscles.
  • The oropharyngeal musculature, which facilitates
    vomiting, works with all of these muscles.

85
Coughing Function
  • Coughing is a reflexive response to irritation of
    laryngeal and tracheal tissues.
  • Afferents mediating irritation initiate the
    coughing reflex via cranial nerve X and the NTS.
  • Diaphragm, abdominal, and intercostal muscles are
    involved, but they contract alternately, not
    simultaneously, as with vomiting.

86
Reticular Functions
  • The functions of the reticular formation can be
    divided into three types cortical arousal,
    sensorimotor elaboration, and visceral integrated
    activity.
  • The activation of cortical arousal are the best
    known functions of the reticular formation.

87
Reticular Functions
  • The reticular formation uses various
    neurotransmitters to communicate with the brain,
    spinal cord, and neighboring reticular regions to
    contribute to cortical arousal.
  • These neurotransmitters are synthesized by a
    specialized population of the cells.

88
Reticular Functions
  • Studies of the brain using histochemical
    techniques have shown that many reticular neurons
    contain biogenic amines and neuroactive peptides
    that are believed to be used as chemical
    messengers.

89
Reticular Functions
  • In sections of a brain that have been exposed to
    radiolabeled transmitter substances, it is
    possible to identify the distinctive fluorescence
    emitted by each of these biogenic amines and to
    map their distribution throughout the reticular
    formation.

90
Reticular Transmitters
  • The three most prominent groups of reticular
    neurons are those that contain norepinephrine,
    dopamine, or serotonin.
  • A monoamine imbalance can generate somatic and
    psychic symptoms of excitement, agitation,
    anxiety, and insomnia.

91
Noradrenergic System
  • Those neurons that contain norepinephrine are
    part of the noradrenergic system.
  • In humans, each locus coeruleus (LC) lying on
    either side of the caudal midbrain and upper
    pons, is made up of approximately 12,000
    noradrenergic neurons that have extensive axonal
    connections with the entire CNS.

92
Noradrenergic System
  • At least five noradrenergic tracts have been
    identified, fanning out from the LC to innervate
    just about every part of the brain.

93
Noradrenergic System
  • All of the cerebral cortex, the thalamus, the
    hypothalamus, the olfactory bulb, the
    hippocampus, the midbrain, the cerebellum and the
    spinal cord receive LC projections.

94
Noradrenergic Functions
  • LC cells seem to be involved in the regulation of
    attention, arousal, and sleep-wake cycles, as
    well as learning, memory, anxiety and pain, mood,
    and brain metabolism.
  • Because of its widespread connections, the LC can
    influence virtually all parts of the brain.

95
Noradrenergic Functions
  • Studies with rats and monkeys have shown that LC
    neurons are activated by new, unexpected,
    non-painful, sensory stimuli in the animals
    environment.
  • They are least active when the animals are not
    vigilant, just sitting around quietly digesting a
    meal.

96
Noradrenergic Functions
  • Therefore, the LC neurons may participate in a
    general arousal of the brain in situations that
    are startling or interesting or that call for
    watchfulness, playing a role in maintaining
    attention and vigilance.
  • They may also have a general function in
    increasing efficiency and responsiveness to
    salient sensory stimuli by speeding information
    processing through point-to-point sensory and
    motor systems.

97
Noradrenergic Functions
  • Noradrenergic projections are known also to
    regulate brain tone by inhibiting background
    activity to enhance the signal-to-noise ratio in
    the brain.
  • Behaviorally, the LC contributes to the
    generation of REM sleep.
  • Therefore, the effects of norepinephrine are
    varied, depending on the part of the brain that
    it activates.

98
Whats love go to do with it?
  • Norepinephrine is associated also with increased
    memory for new stimuli.
  • It has also been associated with imprinting, the
    curious animal habit of doggedly concentrating
    ones attention on another and following this
    individual everywhere that he or she wanders.

99
Whats love go to do with it?
  • Infatuation may be a human form of imprinting.
  • Moreover, increasing levels of norepinephrine
    could explain why the lover can remember the
    smallest details of the beloveds actions and
    vividly remember novel moments spent together.

100
Whats love go to do with it?
  • Finally, increasing levels of norepinephrine also
    produce exhilaration, excessive energy,
    sleeplessness, and loss of appetitesome of the
    basic characteristics of romantic love.

101
Serotonergic System
  • The clusters of serotonergic neurons are found
    along the raphe.
  • Each of these nine nuclei projects to different
    regions of the brain.
  • The more caudal, in the medulla, innervate the
    spinal cord, where they modulate pain-related
    sensory signals.
  • Those more rostral, in the pons and midbrain,
    innervate most of the brain much the same way as
    do the LC neurons.

102
Serotonergic System
  • Specifically, serotonin pathways supply the
    hippocampus, the frontal lobes, the caudate and
    putamen, the hypothalamus, and thalamus.

103
Serotonergic System
  • Similar to LC neurons, raphe nuclei cells fire
    most rapidly during wakefulness, when the animal
    is aroused and active and they are quietest
    during sleep.
  • These neurons seem to be intimately involved in
    the control of sleep-wake cycles as well as the
    different stages of sleep.

104
Serotonergic System
  • Serotonin raphe neurons have also been implicated
    in the control of mood and certain types of
    emotional behavior.
  • Human studies suggest that having normal to
    slightly higher levels of serotonin function may
    tend to translate into a number of socially
    useful, salutary effects on mood and behavior.

105
Serotonergic System
  • High levels of serotonin can be useful for
    multi-tasking, but they can play havoc on ones
    libido.
  • In contrast, low serotonin levels correlate with
    depression and well as impulsivity.

106
Serotonergic System
  • Doctors who treat individuals with most forms of
    obsessive-compulsive disorder prescribe slective
    serotonin reuptake inhibitors (SSRIs) like Prozac
    or Zoloft to elevate levels of serotonin in the
    brain.

107
Whats love got to do with it?
  • A striking symptom of romantic love is incessant
    thinking about the beloved.
  • Lovers cannot turn off their racing thoughts.
  • Their obsessive cogitation about the beloved is
    thought to be due to decreased brain serotonin.

108
Whats love got to do with it?
  • All those countless hours when your mind races
    like a mouse upon a treadmill is probably due to
    a negative relationship between serotonin and its
    relatives, dopamine and norepinephrine.
  • As levels of dopamine and norepinephrine climb,
    they can cause serotonin levels to plummet.

109
Whats love got to do with it?
  • This could explain why a lovers increasing
    romantic ecstasy actually intensifies the
    compulsion to daydream, fantasize, muse, ponder,
    obsess about a romantic partner.

110
Dopaminergic System
  • The dopaminergic (DA) nuclei of the reticular
    formation are located in the midbrain.
  • The substantia nigra, with its darkly pigmented
    cell bodies, projects to the motoric nuclei of
    the basal ganglia to facilitate the initiation of
    voluntary movement.

111
Dopaminergic System
  • Specifically, the projections from the substantia
    nigra to the caudate nucleus and the putamen
    (collectively known as the striatum) are referred
    to as nigrostriatal or mesostriatal projections
    reflecting their midbrain origin.
  • The second dopaminergic source is the ventral
    tegmental area (VTA).

112
Dopaminergic System
  • The VTA is a mother lode for dopamine-making
    cells.
  • With their tentacle-like axons, these nerve cells
    distribute dopamine to many brain regions
    including the caudate nucleus.
  • It has projections to limbic structures such as
    the amygdala via mesolimbic fibers and to the
    cerebral cortex via mesocortical fibers.

113
Dopaminergic System
  • The nigrostriatal projection and the mesocortical
    projections to the motor cortex are both
    consistent with the idea that the DA system is
    involved in the initiation of movement.

114
Dopaminergic System
  • Disruption in these pathways, or degeneration of
    DA-producing cells, is instrumental in the
    movement deficits of Parkinsons disease.
  • However, the extensive DA projections to limbic
    structures and other cortical areas suggest that
    this system is also involved in motivation and
    cognition.

115
Dopaminergic System
  • Elevated levels of dopamine in the brain produce
    extremely focused attention, as well as
    unwavering motivation and goal-directed behavior.
  • When a reward is delayed, dopamine-producing
    cells in the brain increase their work, pumping
    out more this natural stimulant to energize the
    brain, focus attention, and drive the pursuer to
    strive even harder to acquire a reward.

116
Dopaminergic System
  • Dopamine has been associated also with learning
    about novel stimuli.
  • Dopamine levels rise when people are in novel
    situations.
  • Imbalances in the DA system are thought to play a
    role in certain forms of mental illness, such as
    schizophrenia and thought disorders.
  • Very high levels of dopamine can make one feel
    anxious, fearful, even panicky.

117
Dopaminergic System
  • Many drugs of abuse enhance the action of DA
    release in limbic structures producing a sense of
    pleasure.
  • Dependency and craving, symptoms of addiction, as
    well as romantic love, are associated with
    elevated levels of dopamine.

118
Whats love got to do with it?
  • The widespread distribution of this sprinkler
    system sends dopamine to many brain parts.
  • It produces focused attention, as well as fierce
    energy, concentrated motivation to attain a
    reward, and the feelings of elation, even
    maniathe core feelings of romantic love.

119
Whats love got to do with it?
  • Lovers intensely focus on the beloved, often to
    the exclusion of all around them.
  • Indeed, they concentrate so relentlessly on the
    positive qualities of the adored one that they
    easily overlook his/her negative traits.

120
Whats love got to do with it?
  • Ecstasy is another trait of lovers that appears
    to be associated with dopamine.
  • Elevated concentrations of dopamine in the brain
    produce exhilaration, as well as many of the
    feelings that lovers reportincreased energy,
    hyperactivity, sleeplessness, loss of appetite,
    trembling, a pounding heart, accelerated
    breathing, and sometimes mania, anxiety, or fear.

121
Whats love got to do with it?
  • Dopamine may explain why love-stricken
    individuals become so dependent on their romantic
    relationship and why they crave emotional union
    with their beloved.
  • Dopamine probably also stimulates the intense
    motivation to see, talk with, and be with the
    beloved.

122
Loves Complex Chemistry
  • Given the properties of these three related
    chemicals in the brain, they probably all play a
    role in human romantic passion
  • The feelings of euphoria, sleeplessness, and loss
    of appetite
  • The lovers intense energy, focused attention,
    driving motivation, and goal-oriented behaviors

123
Loves Complex Chemistry
  • The lovers tendency to regard the beloved as
    novel and unique and
  • The lovers increased passion in the face of
    adversity.
  • Nonetheless, passionate romantic love takes a
    variety of graded forms, from pure elation when
    ones love is reciprocated to feelings of
    emptiness, despair, and often rage when ones
    love is thwarted.

124
Loves Complex Chemistry
  • These chemicals undoubtedly vary in their
    concentrations and combinations as the
    relationship ebbs and flows.
  • When ones passion is returned, the brain tacks
    on positive emotions, such as elation and hope.
  • When ones love is spurned or thwarted instead,
    the brain links this motivation with negative
    feelings, such as despair and rage.

125
The Drive to Love
  • Neuroscientist Don Pfaff (1999) defines a drive
    as a neural state that energizes and directs
    behavior to acquire a particular biological need
    to survive or reproduce.
  • Drives involve primary motivation systems
    oriented around planning and pursuit of a
    specific want or need.
  • We need food. We need water. We need warmth.

126
The Drive to Love
  • Like all other drives, romantic love is a need, a
    craving, and the lover feels he/she needs the
    beloved.
  • All drives have two components
  • a generalized arousal system and
  • a specific constellation of brain systems to
    produce the feelings, thoughts, and behaviors
    associated with each particular biological need.

127
The Drive to Love
  • The general arousal component of all drives is
    associated with the action of dopamine,
    norepinephrine, serotonin, acetylcholine, several
    histamines, and perhaps other brain chemicals.
  • The specific constellation of brain regions and
    systems associated with each particular drive
    varies considerably.

128
The Drive to Love
  • In their fMRI study, Helen Fisher and her
    colleagues (2003) found the general arousal
    component of romantic love associated with the
    VTA and the distribution of central dopamine.
  • They also found activation in the caudate body
    and tail, the septum, white matter of the
    posterior cingulate, and other areas, as well as
    deactivations in several brain regions.

129
The Drive to Love
  • These areas may constitute part of the system
    specific to intense, early stage romantic love.
  • In addition to brain system chemistry, the
    prefrontal cortex is also hypothesized to be
    involved.
  • This central executive collects data from our
    senses, weighs them, integrates thoughts with
    feelings, makes choices, and controls our basic
    drives.

130
The Drive to Love
  • Because romantic love is focused on a specific
    rewardthe beloved--it constitutes a primary
    motivation system.
  • Several regions of the prefrontal cortex are
    associated with monitoring rewards (Schultz,
    2000).
  • With respect to love, the orbitofrontal and the
    medial prefrontal cortices are specifically
    involved.

131
The Drive to Love
  • The orbitofrontal cortex is involved in
    detecting, perceiving, and expecting rewards, as
    well as discriminating between rewards and making
    preferences.
  • The medial prefrontal cortex experiences
    emotions, bestows meaning to our perceptions,
    guides our reward-related behaviors, creates our
    mood, and also makes preferences.

132
The Drive to Love
  • The drive to love, then, is an elegant design.
  • The passion of love emanates from the motor of
    the mind, the caudate nucleus.
  • It is fueled by at least one of natures most
    powerful stimulants, dopamine.
  • When ones passion is returned, the brain tacks
    on positive emotions, such as elation and hope.

133
The Drive to Love
  • When ones love is spurned or thwarted instead,
    the brain links this motivation with negative
    feelings, such as despair and rage.
  • And all the while, regions of the prefrontal
    cortex monitor the pursuit, planning tactics,
    calculating gains and losses, and registering
    ones progress toward the goal emotional,
    physical, even spiritual union with the beloved.

134
The Drive to Love
  • Indeed, this three-pound blob can generate a need
    so intense that all the world has sung of it
    romantic love.
  • And to make our lives even more complex, romantic
    passion is intricately enmeshed with two other
    basic mating drives, the sex drive and the urge
    to build a deep attachment to a romantic partner
    (Fisher, 2004).
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