Entry - #173100 - ISOLATED GROWTH HORMONE DEFICIENCY, TYPE II; IGHD2 - OMIM - (MIRROR)

 
ICD+
# 173100

ISOLATED GROWTH HORMONE DEFICIENCY, TYPE II; IGHD2


Alternative titles; symbols

IGHD II
GROWTH HORMONE DEFICIENCY, ISOLATED, AUTOSOMAL DOMINANT
PITUITARY DWARFISM DUE TO ISOLATED GROWTH HORMONE DEFICIENCY, AUTOSOMAL DOMINANT


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
17q23.3 Growth hormone deficiency, isolated, type II 173100 AD 3 GH1 139250
Clinical Synopsis
 
Phenotypic Series
 

Growth
- Dwarfism
Endocrine
- Isolated growth hormone deficiency
Lab
- Insulin responses to glucose and to arginine usually greater than normal
- No insulinopenia
Inheritance
- Autosomal dominant form
▲ Close

TEXT

A number sign (#) is used with this entry because of evidence that isolated growth hormone deficiency type II (IGHD2) is caused by heterozygous mutation in the GH1 gene (139250) on chromosome 17q23.

Description

Type II IGHD is an autosomal dominant disorder characterized by low but detectable levels of growth hormone (GH), variable height deficit and age at presentation, and good response to rhGH. Patients may show anterior pituitary hypoplasia on MRI (summary by Phillips and Cogan, 1994; Alatzoglou and Dattani, 2012).


Clinical Features

Phillips and Cogan (1994) referred to the autosomal dominant form of isolated growth hormone deficiency as IGHD II. They pointed out that the clinical severity varies considerably between kindreds and that affected patients respond well to GH treatment without the development of antibodies.

Merimee et al. (1969) and Tyson (1971) observed a family with affected persons in 4 generations. Dominant inheritance seems possible in the case of those patients who have isolated growth hormone deficiency but do not have insulinopenia as is found in most such cases. Unlike type I isolated growth hormone deficiency (see 262400), insulin responses to glucose and to arginine are usually greater than normal.

Tani et al. (1987) described 5 cases of isolated growth hormone deficiency in 3 successive generations. The 3 patients who were so studied had no abnormality of their growth hormone genes on Southern blot analysis. CT scans showed empty sella. Growth hormone was detectable in the plasma by radioimmunoassay but levels were clearly lower than in normal children, and significant increases were not obtained with the insulin tolerance test or with the arginine-TRH-LHRH triple loading test. Repeated injections of growth hormone releasing factor (GHRF; 139190) had no effect.

In a high proportion of patients with isolated growth hormone deficiency and multiple pituitary hormone deficiency, characteristic radiologic findings include (1) a small or absent anterior pituitary gland, (2) a small or truncated infundibulum, and (3) an ectopic posterior pituitary hyperintensity located at the base of the hypothalamus or inferior end of the truncated pituitary stalk. These findings have been attributed to a developmental defect, trauma, or ischemia at birth. Hamilton et al. (1998) described isolated growth deficiency in mother and son with characteristic findings on magnetic resonance imaging. The son also had a Chiari type I malformation and medial deviation of the carotid arteries secondary to a narrow skull base. Testing failed to identify a mutation in either the PIT1 gene (173110) or the growth hormone gene cluster. The authors interpreted the case as one of autosomal dominant defect in early development, lending support to the hypothesis that dysgenesis, rather than birth trauma, may cause a small anterior pituitary and ectopic posterior pituitary.


Inheritance

Numerous reports support autosomal dominant inheritance of a form of isolated growth hormone deficiency. Persons who appear to have had isolated growth hormone deficiency have been observed in successive generations. Selle (1920) is said (Warkany et al., 1961) to have described a kindred in which 'primordial dwarfism' was transmitted through 3 generations, 10 persons being affected. Multigeneration kindreds were included in the review of Rischbieth and Barrington (1912).

Dominant inheritance is a possible explanation for the findings in a family in which 2 dwarf parents with demonstrated isolated growth hormone deficiency have 3 offspring, 2 with dwarfism and 1 of normal stature (Rimoin et al., 1966). The father's condition may have been the result of new dominant mutation and he may have transmitted the condition to the 2 affected offspring.

Sheikholislam and Stempfel (1972) reported isolated GH deficiency in a man and 3 daughters and a son. Three other children were unaffected. Pedigree patterns consistent with dominant inheritance were reported also by Butenandt and Knorr (1970) and by Sadeghi-Nejad and Senior (1974). (The latter report concerned association with Rieger syndrome (180500).)

Poskitt and Rayner (1974) described 2 families, each with a father and son affected by isolated GH deficiency.

Rona and Tanner (1977) described an affected parent and 2 children with no known consanguinity.

Van Gelderen and van der Hoog (1981) reported isolated GH deficiency in 2 girls and their mother. Two maternal uncles, 135 cm tall, and the maternal grandmother were presumably affected also. The mother's height was 133 cm.


Cytogenetics

Schober et al. (1995) described growth hormone deficiency and empty sella in a 6-year-old girl with 18p monosomy. Good response to growth hormone treatment was observed. A rudimentary pituitary stalk was considered to underlie the hormone deficiency. The association of growth hormone deficiency and pituitary hypoplasia in 18p monosomy was also found by Artman et al. (1992). In addition to short stature, the craniofacial features of 18p monosomy may resemble those of Turner syndrome: round face, hypertelorism, flattened nasal bridge, and wide mouth with small upper lip. Various degrees of mental retardation have been observed.


Molecular Genetics

Most mutations leading to type II IGHD have been shown to affect the correct splicing of GH1, and in the majority of cases they are single base mutations within the first 6 nucleotides of intron 3. The result is the skipping of exon 3 and the production of the 17.5-kD isoform that exerts a dominant-negative effect on the secretion of the 22-kD molecule (summary by Alatzoglou and Dattani, 2012).

In affected members of a Turkish family segregating IGHD II, Phillips and Cogan (1994) identified a splice site mutation in the GH1 gene (IVS3+6T-C; 139250.0007).

Mullis et al. (2005) studied a total of 57 subjects with IGHD II belonging to 19 families with different splice site as well as missense mutations within the GH1 gene. The subjects presenting with the splice site mutation within the first 2 bp of intervening sequence 3 (139250.0009) leading to a skipping of exon 3 were more likely to present in the follow-up with other pituitary hormone deficiencies. In addition, although the patients with missense mutations had been reported to be less affected, a number of patients presenting with a missense GH form showed some pituitary hormone impairment. The development of multiple hormonal deficiencies is not age-dependent, and there is a clear variability in onset, severity, and progression, even within the same families. Mullis et al. (2005) concluded that the message of clinical importance from these studies is that the pituitary endocrine status of all such patients should continue to be monitored closely over the years because further hormonal deficiencies may evolve with time.

Shariat et al. (2008) studied a 4-generation family with IGHD II and identified a heterozygous missense mutation in the GH1 gene (EX3+1G-A; 139250.0025) in affected individuals. Functional analysis of this variant as well as G-T and G-C changes at the first nucleotide of exon 3 illustrated the multiple mechanisms by which changes in sequence can cause disease: splice site mutations, splicing enhancer function, messenger RNA decay, missense mutations, and nonsense mutations. The authors noted that for IGHD II, only exon skipping leads to production of the dominant-negative isoform, with increasing skipping correlating with increasing disease severity.


REFERENCES

  1. Alatzoglou, K. S., Dattani, M. T. Phenotype-genotype correlations in congenital isolated growth hormone deficiency (IGHD). Indian J. Pediat. 79: 99-106, 2012. [PubMed: 22139958, related citations] [Full Text]

  2. Artman, H. G., Morris, C. A., Stock, A. D. 18p- syndrome and hypopituitarism. J. Med. Genet. 29: 671-672, 1992. [PubMed: 1404301, related citations] [Full Text]

  3. Butenandt, O., Knorr, D. Familiaerer Hypopituitarismus. Mschr. Kinderheilk. 118: 470-473, 1970. [PubMed: 5511839, related citations]

  4. Gertner, J. M., Genel, M., Arulanantham, K., Crawford, J. D. Dominant inheritance of isolated growth hormone deficiency transmitted through an individual of normal stature. (Abstract) Pediat. Res. 12: 451, 1978.

  5. Hamilton, J., Chitayat, D., Blaser, S., Cohen, L. E., Phillips, J. A., III, Daneman, D. Familial growth hormone deficiency associated with MRI abnormalities. Am. J. Med. Genet. 80: 128-132, 1998. [PubMed: 9805128, related citations]

  6. Merimee, T. J., Hall, J. G., Rimoin, D. L., McKusick, V. A. A metabolic and hormonal basis for classifying ateliotic dwarfs. Lancet 293: 963-965, 1969. Note: Originally Volume I. [PubMed: 4180815, related citations] [Full Text]

  7. Merimee, T. J. Studies in HGH-deficient dwarfs: the type II anomaly. Johns Hopkins Med. J. 131: 165-171, 1972. [PubMed: 5050736, related citations]

  8. Mullis, P. E., Robinson, I. C. A. F., Salemi, S., Eble, A., Besson, A., Vuissoz, J.-M., Deladoey, J., Simon, D., Czernichow, P., Binder, G. Isolated autosomal dominant growth hormone deficiency: an evolving pituitary deficit? A multicenter follow-up study. J. Clin. Endocr. Metab. 90: 2089-2096, 2005. [PubMed: 15671105, related citations] [Full Text]

  9. Phillips, J. A., III, Cogan, J. D. Genetic basis of endocrine disease 6: molecular basis of familial human growth hormone deficiency. J. Clin. Endocr. 78: 11-16, 1994. [PubMed: 8288694, related citations] [Full Text]

  10. Poskitt, E. M. E., Rayner, P. H. W. Isolated growth hormone deficiency: two families with autosomal dominant inheritance. Arch. Dis. Child. 49: 55-59, 1974. [PubMed: 4361890, related citations] [Full Text]

  11. Rimoin, D. L., Merimee, T. J., McKusick, V. A. Growth hormone deficiency in man: an isolated recessively inherited defect. Science 152: 1635-1637, 1966. [PubMed: 4287048, related citations] [Full Text]

  12. Rischbieth, H., Barrington, A. Dwarfism. In: Pearson, K. (ed.): Treasury of Human Inheritance. Vol. 1. Part 7. Sec. 15A. London: Dulau and Co. (pub.) 1912. P. 355.

  13. Rona, R. J., Tanner, J. M. Aetiology of idiopathic growth hormone deficiency in England and Wales. Arch. Dis. Child. 52: 197-208, 1977. [PubMed: 848998, related citations] [Full Text]

  14. Sadeghi-Nejad, A., Senior, B. Autosomal dominant transmission of isolated growth hormone deficiency in iris-dental dysplasia (Rieger's syndrome). J. Pediat. 85: 644-648, 1974. [PubMed: 4214375, related citations] [Full Text]

  15. Schober, E., Scheibenreiter, S., Frisch, H. 18p monosomy with GH-deficiency and empty sella: good response to GH-treatment. Clin. Genet. 47: 254-256, 1995. [PubMed: 7554351, related citations] [Full Text]

  16. Selle, G. Ueber Vererbung des echten Zwergwuchses. Inaug. Dissert.: Univ. of Jena (pub.) 1920.

  17. Shariat, N., Holladay, C. D., Cleary, R. K., Phillips, J. A., III, Patton, J. G. Isolated growth hormone deficiency type II caused by a point mutation that alters both splice site strength and splicing enhancer function. Clin. Genet. 74: 539-545, 2008. [PubMed: 18554279, images, related citations] [Full Text]

  18. Sheikholislam, B. M., Stempfel, R. S., Jr. Hereditary isolated somatotropin deficiency: effects of human growth hormone administration. Pediatrics 49: 362-374, 1972. [PubMed: 5010465, related citations]

  19. Tani, N., Kaneko, K., Momotsu, T., Takasawa, T., Ito, S., Shibata, A., Miki, T., Tateishi, H., Kumahara, Y. A family case with autosomal-dominantly inherited pituitary dwarfism. Tohoku J. Exp. Med. 152: 319-324, 1987. [PubMed: 3660403, related citations] [Full Text]

  20. Tyson, J. E. A. Isolated growth hormone deficiency, type I (sexual ateleiosis, type I). Birth Defects Orig. Art. Ser. VII(6): 251-252, 1971.

  21. van Gelderen, H. H., van der Hoog, C. E. Familial isolated growth hormone deficiency. Clin. Genet. 20: 173-175, 1981. [PubMed: 7307312, related citations] [Full Text]

  22. Warkany, J., Monroe, B. B., Sutherland, B. S. Intrauterine growth retardation. Am. J. Dis. Child. 102: 249-279, 1961. [PubMed: 13783175, related citations] [Full Text]


Contributors:
Marla J. F. O'Neill - updated : 3/30/2009
John A. Phillips, III - updated : 7/21/2006
Victor A. McKusick - updated : 12/4/1998
John A. Phillips, III - updated : 3/5/1996
Creation Date:
Victor A. McKusick : 6/2/1986
Edit History:
carol : 10/25/2018
carol : 10/14/2016
alopez : 06/05/2009
alopez : 6/2/2009
carol : 3/31/2009
terry : 3/30/2009
terry : 2/6/2009
alopez : 7/21/2006
alopez : 7/21/2006
carol : 11/9/1999
carol : 12/9/1998
terry : 12/4/1998
dkim : 9/11/1998
alopez : 6/2/1997
jenny : 4/1/1997
mark : 2/25/1997
terry : 2/24/1997
carol : 10/7/1996
joanna : 4/19/1996
joanna : 3/5/1996
mark : 7/12/1995
mimadm : 1/14/1995
pfoster : 4/5/1994
warfield : 3/29/1994
carol : 3/24/1994
supermim : 3/16/1992

# 173100

ISOLATED GROWTH HORMONE DEFICIENCY, TYPE II; IGHD2


Alternative titles; symbols

IGHD II
GROWTH HORMONE DEFICIENCY, ISOLATED, AUTOSOMAL DOMINANT
PITUITARY DWARFISM DUE TO ISOLATED GROWTH HORMONE DEFICIENCY, AUTOSOMAL DOMINANT


SNOMEDCT: 237687003;   ORPHA: 231679, 631;   DO: 0060872;  


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
17q23.3 Growth hormone deficiency, isolated, type II 173100 Autosomal dominant 3 GH1 139250

TEXT

A number sign (#) is used with this entry because of evidence that isolated growth hormone deficiency type II (IGHD2) is caused by heterozygous mutation in the GH1 gene (139250) on chromosome 17q23.

Description

Type II IGHD is an autosomal dominant disorder characterized by low but detectable levels of growth hormone (GH), variable height deficit and age at presentation, and good response to rhGH. Patients may show anterior pituitary hypoplasia on MRI (summary by Phillips and Cogan, 1994; Alatzoglou and Dattani, 2012).


Clinical Features

Phillips and Cogan (1994) referred to the autosomal dominant form of isolated growth hormone deficiency as IGHD II. They pointed out that the clinical severity varies considerably between kindreds and that affected patients respond well to GH treatment without the development of antibodies.

Merimee et al. (1969) and Tyson (1971) observed a family with affected persons in 4 generations. Dominant inheritance seems possible in the case of those patients who have isolated growth hormone deficiency but do not have insulinopenia as is found in most such cases. Unlike type I isolated growth hormone deficiency (see 262400), insulin responses to glucose and to arginine are usually greater than normal.

Tani et al. (1987) described 5 cases of isolated growth hormone deficiency in 3 successive generations. The 3 patients who were so studied had no abnormality of their growth hormone genes on Southern blot analysis. CT scans showed empty sella. Growth hormone was detectable in the plasma by radioimmunoassay but levels were clearly lower than in normal children, and significant increases were not obtained with the insulin tolerance test or with the arginine-TRH-LHRH triple loading test. Repeated injections of growth hormone releasing factor (GHRF; 139190) had no effect.

In a high proportion of patients with isolated growth hormone deficiency and multiple pituitary hormone deficiency, characteristic radiologic findings include (1) a small or absent anterior pituitary gland, (2) a small or truncated infundibulum, and (3) an ectopic posterior pituitary hyperintensity located at the base of the hypothalamus or inferior end of the truncated pituitary stalk. These findings have been attributed to a developmental defect, trauma, or ischemia at birth. Hamilton et al. (1998) described isolated growth deficiency in mother and son with characteristic findings on magnetic resonance imaging. The son also had a Chiari type I malformation and medial deviation of the carotid arteries secondary to a narrow skull base. Testing failed to identify a mutation in either the PIT1 gene (173110) or the growth hormone gene cluster. The authors interpreted the case as one of autosomal dominant defect in early development, lending support to the hypothesis that dysgenesis, rather than birth trauma, may cause a small anterior pituitary and ectopic posterior pituitary.


Inheritance

Numerous reports support autosomal dominant inheritance of a form of isolated growth hormone deficiency. Persons who appear to have had isolated growth hormone deficiency have been observed in successive generations. Selle (1920) is said (Warkany et al., 1961) to have described a kindred in which 'primordial dwarfism' was transmitted through 3 generations, 10 persons being affected. Multigeneration kindreds were included in the review of Rischbieth and Barrington (1912).

Dominant inheritance is a possible explanation for the findings in a family in which 2 dwarf parents with demonstrated isolated growth hormone deficiency have 3 offspring, 2 with dwarfism and 1 of normal stature (Rimoin et al., 1966). The father's condition may have been the result of new dominant mutation and he may have transmitted the condition to the 2 affected offspring.

Sheikholislam and Stempfel (1972) reported isolated GH deficiency in a man and 3 daughters and a son. Three other children were unaffected. Pedigree patterns consistent with dominant inheritance were reported also by Butenandt and Knorr (1970) and by Sadeghi-Nejad and Senior (1974). (The latter report concerned association with Rieger syndrome (180500).)

Poskitt and Rayner (1974) described 2 families, each with a father and son affected by isolated GH deficiency.

Rona and Tanner (1977) described an affected parent and 2 children with no known consanguinity.

Van Gelderen and van der Hoog (1981) reported isolated GH deficiency in 2 girls and their mother. Two maternal uncles, 135 cm tall, and the maternal grandmother were presumably affected also. The mother's height was 133 cm.


Cytogenetics

Schober et al. (1995) described growth hormone deficiency and empty sella in a 6-year-old girl with 18p monosomy. Good response to growth hormone treatment was observed. A rudimentary pituitary stalk was considered to underlie the hormone deficiency. The association of growth hormone deficiency and pituitary hypoplasia in 18p monosomy was also found by Artman et al. (1992). In addition to short stature, the craniofacial features of 18p monosomy may resemble those of Turner syndrome: round face, hypertelorism, flattened nasal bridge, and wide mouth with small upper lip. Various degrees of mental retardation have been observed.


Molecular Genetics

Most mutations leading to type II IGHD have been shown to affect the correct splicing of GH1, and in the majority of cases they are single base mutations within the first 6 nucleotides of intron 3. The result is the skipping of exon 3 and the production of the 17.5-kD isoform that exerts a dominant-negative effect on the secretion of the 22-kD molecule (summary by Alatzoglou and Dattani, 2012).

In affected members of a Turkish family segregating IGHD II, Phillips and Cogan (1994) identified a splice site mutation in the GH1 gene (IVS3+6T-C; 139250.0007).

Mullis et al. (2005) studied a total of 57 subjects with IGHD II belonging to 19 families with different splice site as well as missense mutations within the GH1 gene. The subjects presenting with the splice site mutation within the first 2 bp of intervening sequence 3 (139250.0009) leading to a skipping of exon 3 were more likely to present in the follow-up with other pituitary hormone deficiencies. In addition, although the patients with missense mutations had been reported to be less affected, a number of patients presenting with a missense GH form showed some pituitary hormone impairment. The development of multiple hormonal deficiencies is not age-dependent, and there is a clear variability in onset, severity, and progression, even within the same families. Mullis et al. (2005) concluded that the message of clinical importance from these studies is that the pituitary endocrine status of all such patients should continue to be monitored closely over the years because further hormonal deficiencies may evolve with time.

Shariat et al. (2008) studied a 4-generation family with IGHD II and identified a heterozygous missense mutation in the GH1 gene (EX3+1G-A; 139250.0025) in affected individuals. Functional analysis of this variant as well as G-T and G-C changes at the first nucleotide of exon 3 illustrated the multiple mechanisms by which changes in sequence can cause disease: splice site mutations, splicing enhancer function, messenger RNA decay, missense mutations, and nonsense mutations. The authors noted that for IGHD II, only exon skipping leads to production of the dominant-negative isoform, with increasing skipping correlating with increasing disease severity.


See Also:

Gertner et al. (1978); Merimee (1972)

REFERENCES

  1. Alatzoglou, K. S., Dattani, M. T. Phenotype-genotype correlations in congenital isolated growth hormone deficiency (IGHD). Indian J. Pediat. 79: 99-106, 2012. [PubMed: 22139958] [Full Text: https://doi.org/10.1007/s12098-011-0614-7]

  2. Artman, H. G., Morris, C. A., Stock, A. D. 18p- syndrome and hypopituitarism. J. Med. Genet. 29: 671-672, 1992. [PubMed: 1404301] [Full Text: https://doi.org/10.1136/jmg.29.9.671]

  3. Butenandt, O., Knorr, D. Familiaerer Hypopituitarismus. Mschr. Kinderheilk. 118: 470-473, 1970. [PubMed: 5511839]

  4. Gertner, J. M., Genel, M., Arulanantham, K., Crawford, J. D. Dominant inheritance of isolated growth hormone deficiency transmitted through an individual of normal stature. (Abstract) Pediat. Res. 12: 451, 1978.

  5. Hamilton, J., Chitayat, D., Blaser, S., Cohen, L. E., Phillips, J. A., III, Daneman, D. Familial growth hormone deficiency associated with MRI abnormalities. Am. J. Med. Genet. 80: 128-132, 1998. [PubMed: 9805128]

  6. Merimee, T. J., Hall, J. G., Rimoin, D. L., McKusick, V. A. A metabolic and hormonal basis for classifying ateliotic dwarfs. Lancet 293: 963-965, 1969. Note: Originally Volume I. [PubMed: 4180815] [Full Text: https://doi.org/10.1016/s0140-6736(69)91861-3]

  7. Merimee, T. J. Studies in HGH-deficient dwarfs: the type II anomaly. Johns Hopkins Med. J. 131: 165-171, 1972. [PubMed: 5050736]

  8. Mullis, P. E., Robinson, I. C. A. F., Salemi, S., Eble, A., Besson, A., Vuissoz, J.-M., Deladoey, J., Simon, D., Czernichow, P., Binder, G. Isolated autosomal dominant growth hormone deficiency: an evolving pituitary deficit? A multicenter follow-up study. J. Clin. Endocr. Metab. 90: 2089-2096, 2005. [PubMed: 15671105] [Full Text: https://doi.org/10.1210/jc.2004-1280]

  9. Phillips, J. A., III, Cogan, J. D. Genetic basis of endocrine disease 6: molecular basis of familial human growth hormone deficiency. J. Clin. Endocr. 78: 11-16, 1994. [PubMed: 8288694] [Full Text: https://doi.org/10.1210/jcem.78.1.8288694]

  10. Poskitt, E. M. E., Rayner, P. H. W. Isolated growth hormone deficiency: two families with autosomal dominant inheritance. Arch. Dis. Child. 49: 55-59, 1974. [PubMed: 4361890] [Full Text: https://doi.org/10.1136/adc.49.1.55]

  11. Rimoin, D. L., Merimee, T. J., McKusick, V. A. Growth hormone deficiency in man: an isolated recessively inherited defect. Science 152: 1635-1637, 1966. [PubMed: 4287048] [Full Text: https://doi.org/10.1126/science.152.3729.1635]

  12. Rischbieth, H., Barrington, A. Dwarfism. In: Pearson, K. (ed.): Treasury of Human Inheritance. Vol. 1. Part 7. Sec. 15A. London: Dulau and Co. (pub.) 1912. P. 355.

  13. Rona, R. J., Tanner, J. M. Aetiology of idiopathic growth hormone deficiency in England and Wales. Arch. Dis. Child. 52: 197-208, 1977. [PubMed: 848998] [Full Text: https://doi.org/10.1136/adc.52.3.197]

  14. Sadeghi-Nejad, A., Senior, B. Autosomal dominant transmission of isolated growth hormone deficiency in iris-dental dysplasia (Rieger's syndrome). J. Pediat. 85: 644-648, 1974. [PubMed: 4214375] [Full Text: https://doi.org/10.1016/s0022-3476(74)80507-x]

  15. Schober, E., Scheibenreiter, S., Frisch, H. 18p monosomy with GH-deficiency and empty sella: good response to GH-treatment. Clin. Genet. 47: 254-256, 1995. [PubMed: 7554351] [Full Text: https://doi.org/10.1111/j.1399-0004.1995.tb04306.x]

  16. Selle, G. Ueber Vererbung des echten Zwergwuchses. Inaug. Dissert.: Univ. of Jena (pub.) 1920.

  17. Shariat, N., Holladay, C. D., Cleary, R. K., Phillips, J. A., III, Patton, J. G. Isolated growth hormone deficiency type II caused by a point mutation that alters both splice site strength and splicing enhancer function. Clin. Genet. 74: 539-545, 2008. [PubMed: 18554279] [Full Text: https://doi.org/10.1111/j.1399-0004.2008.01042.x]

  18. Sheikholislam, B. M., Stempfel, R. S., Jr. Hereditary isolated somatotropin deficiency: effects of human growth hormone administration. Pediatrics 49: 362-374, 1972. [PubMed: 5010465]

  19. Tani, N., Kaneko, K., Momotsu, T., Takasawa, T., Ito, S., Shibata, A., Miki, T., Tateishi, H., Kumahara, Y. A family case with autosomal-dominantly inherited pituitary dwarfism. Tohoku J. Exp. Med. 152: 319-324, 1987. [PubMed: 3660403] [Full Text: https://doi.org/10.1620/tjem.152.319]

  20. Tyson, J. E. A. Isolated growth hormone deficiency, type I (sexual ateleiosis, type I). Birth Defects Orig. Art. Ser. VII(6): 251-252, 1971.

  21. van Gelderen, H. H., van der Hoog, C. E. Familial isolated growth hormone deficiency. Clin. Genet. 20: 173-175, 1981. [PubMed: 7307312] [Full Text: https://doi.org/10.1111/j.1399-0004.1981.tb01824.x]

  22. Warkany, J., Monroe, B. B., Sutherland, B. S. Intrauterine growth retardation. Am. J. Dis. Child. 102: 249-279, 1961. [PubMed: 13783175] [Full Text: https://doi.org/10.1001/archpedi.1961.02080010251018]


Contributors:
Marla J. F. O'Neill - updated : 3/30/2009
John A. Phillips, III - updated : 7/21/2006
Victor A. McKusick - updated : 12/4/1998
John A. Phillips, III - updated : 3/5/1996

Creation Date:
Victor A. McKusick : 6/2/1986

Edit History:
carol : 10/25/2018
carol : 10/14/2016
alopez : 06/05/2009
alopez : 6/2/2009
carol : 3/31/2009
terry : 3/30/2009
terry : 2/6/2009
alopez : 7/21/2006
alopez : 7/21/2006
carol : 11/9/1999
carol : 12/9/1998
terry : 12/4/1998
dkim : 9/11/1998
alopez : 6/2/1997
jenny : 4/1/1997
mark : 2/25/1997
terry : 2/24/1997
carol : 10/7/1996
joanna : 4/19/1996
joanna : 3/5/1996
mark : 7/12/1995
mimadm : 1/14/1995
pfoster : 4/5/1994
warfield : 3/29/1994
carol : 3/24/1994
supermim : 3/16/1992



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.
Printed: Nov. 30, 2024