. 2020 Mar 28;140(1):113–134. doi: 10.1007/s00439-020-02148-0

Table 4.

Variants identified by targeted NGS panel in 38 CHH probands

Patient ID	Sex	Clinical diagnosis	Gene_name	Inheritance	Variant identified			ACMG classification	Minor allele frequency (MAF)		Prediction (DANN)	Gene Reference	Variant Reference (HGMD ID, Ref)
Patient ID	Sex	Clinical diagnosis	Gene_name	Inheritance	HGVS cdna	HGVS prot	Zygosity	ACMG classification	Total	Eu (non-Finnish)	Prediction (DANN)	Gene Reference	Variant Reference (HGMD ID, Ref)
Probands (n = 38)
3	F	KS, anosmia (primer amenorrhea)	PROKR2	AD, contributes to oligogenicity	NM_144773.3:c.518 T > G	p.Leu173Arg	Heterozygous	Likely pathogenic	0.00229	0.00347	0.9976	Boehm et al. (2015)	Dodé et al. (2006), Cole et al. (2008), Monnier et al. (2009), Abreu et al. (2010), Reynaud et al. (2012), Cassatella et al. (2018), Amato et al. (2019)
5	M	KS	AMH	AR (Malone et al. 2019)	NM_000479.4:c.1556C > T	p.Ala519Val	Heterozygous	VUS	0.00159	0.00252	0.9582	Malone et al. (2019)	Novel in IHH (It was deteceted in a DSD case by Hughes et al. (2019))
5	M	KS	JAG1	AD (Quaynor et al. 2016)	NM_000214.3:c.3109G > A	p.Asp1037Asn	Heterozygous	VUS	0.00000795	0.0000176	0.9918	Quaynor et al. (2016)	Novel in IHH
10	M	KS, anosmia, pubertal delay	FGFR1	AD, contributes to oligogenicity	NM_001174067.1:c.417delC^a	p.Ser140ArgfsTer43	heterozygous	Pathogenic	Absent	Absent	na	Boehm et al. (2015)	Novel in IHH
10	M	KS, anosmia, pubertal delay	IL17RD	AD, AR or digenic dominant, contributes to oligogenicity	NM_017563.5:c.1696C > T	p.Pro566Ser	Heterozygous	VUS	0.0144	0.0214	0.9981	Boehm et al. (2015)	Novel in IHH [Amato et al. (2019) found a pathogenic variant in the same codon: c.1697C > T; p.Pro566Leu]
12	M		PDE3A	Digenic (Quaynor et al. 2016)	NM_000921.4:c.293C > A	p.Ala98Glu	Heterozygous	VUS	0.000431	0.000884	0.7627	Quaynor et al. (2016)	Novel in IHH
13	M	KS	ANOS1	XR, contributes to oligogenicity	NM_000216.4:c.1700G > A	p.Gly567Asp	Hemizygous	Likely pathogenic	Absent	Absent	0.9959	Boehm et al. (2015)	Novel in IHH
15	M	KS, anosmia, parosmia	GNRHR	AR, contributes to oligogenicity	NM_000406.2:c.416G > A	p.Arg139His	Heterozygous	Likely pathogenic	0.000144	0.000168	0.9994	Boehm et al. (2015)	Costa et al. (2001), Topaloglu et al. (2006), Beneduzzi et al. (2014)
16	M	KS	GLI3	digenic (Quaynor et al. 2016)	NM_000168.6:c.2179G > A	p.Gly727Arg	Heterozygous	VUS	0.00527	0.00755	0.9994	Quaynor et al. (2016)	Novel in IHH (Radhakrishna et al. 1999 detected in postaxial polydactyly type-A/B)
16	M	KS	JAG1	AD (Quaynor et al. 2016)	NM_000214.3:c.3320C > T	p.Ser1107Phe	Heterozygous	VUS	Absent	Absent	0.9929	Quaynor et al. (2016)	Novel in IHH
17	M	KS	NOTCH1	AD? (Quaynor et al. 2016)	NM_017617.5:c.4049G > T	p.Arg1350Leu	Heterozygous	VUS	0.000604	0.00103	0.6583	Quaynor et al. (2016)	Novel in IHH
18	M	nCHH, pubertal delay	GLI3	digenic (Quaynor et al. 2016)	NM_000168.6:c.2179G > A	p.Gly727Arg	Heterozygous	VUS	0.00527	0.00755	0.9994	Quaynor et al. 2016	Novel in IHH [Radhakrishna et al. (1999) detected in postaxial polydactyly type-A/B]
20	M	KS, anosmia, pubertal delay	NOTCH1	AD? (Quaynor et al. 2016)	NM_017617.5:c.3860G > A	p.Arg1287His	Heterozygous	VUS	0.0000688	0.000191	0.9977	Quaynor et al. (2016)	Novel in IHH
23	M	KS, anosmia	FGFR1	AD, contributes to oligogenicity	NM_001174067.1:c.1012delT^a	p.Tyr338MetfsTer5	Heterozygous	Pathogenic	–	–	na	Boehm et al. (2015)	Novel in IHH
26	M	nCHH, pubertal delay	MASTL	AD, di-, trigenic (Quaynor et al. 2016)	NM_001172303.2:c.2120A > T	p.His707Leu	Heterozygous	VUS	0.000004	0.000000	0.8767	Quaynor et al. (2016)	Novel in IHH
26	M	nCHH, pubertal delay	TAC3	AR, contributes to oligogenicity	NM_013251.4:c.248A>C	p.His83Pro	heterozygous	VUS	0.000008	0.000009	0.977	Boehm et al. (2015)	Novel in IHH [Cassatella et al. (2018) found a pathogenic variant in the same codon: c.248A>G; p.His83Arg]
29	M	nCHH	GNRHR	AR, contributes to oligogenicity	NM_000406.2:c.350 T > G	p.Leu117Arg	Heterozygous	Likely pathogenic	absent	absent	0.9971	Boehm et al. (2015)	HGMD ID: CM128135 Gürbüz et al. (2012), Cassatella et al. (2018)
29	M	nCHH	GNRHR	AR, contributes to oligogenicity	NM_000406.2:c.158A > T	p.Asn53Ile	Heterozygous	VUS	Absent	Absent	0.9881	Boehm et al. (2015)	Novel in IHH
30	M	nCHH	NOTCH1	AD? (Quaynor et al. 2016)	NM_017617.5:c.2734C > T	p.Arg912Trp	Heterozygous	VUS	0.001710	0.002570	0.9989	Quaynor et al. (2016)	Novel in IHH [Digilio et al. (2019) reported in association with cardiovascular anomalies]
30	M	nCHH	PROKR2	AD, contributes to oligogenicity	NM_144773.3:c.701G > A	p.Gly234Asp	Heterozygous	VUS	0.000008	0.000018	0.9981	Boehm et al. (2015)	HGMD ID: CM1211225 Tommiska et al. (2013)
31	M	KS, hyposmia	ANOS1	XR, contributes to oligogenicity	NM_000216.4:c.1246dupA^a	p.Thr416AsnfsTer29	Hemizygous	Pathogenic	–	–	na	Boehm et al. (2015)	Novel in IHH
31	M	KS, hyposmia	MASTL	AD, di-, trigenic (Quaynor et al. 2016)	NM_001172303.2:c.871C > T	p.Leu291Phe	Heterozygous	VUS	0.000540	0.000940	0.9989	Quaynor et al. (2016)	Novel in IHH
32	M	nCHH, pubertal delay	TACR3	AR, contributes to oligogenicity	NM_001059.2:c.1345G>T	p.Ala449Ser	Heterozygous	VUS	0.000162	0.000305	0.9737	Boehm et al. (2015)	Tusset et al (2012) reported in a case of CDGP
33	M	nCHH, pubertal delay	AMHR2	AR (Malone et al. 2019)	NM_020547.3:c.1484G > A	p.Arg495Gln	Heterozygous	Likely pathogenic^a	0.000203	0.000009	0.9995	Malone et al. (2019)	Novel in IHH
35	M	pubertal delay	KISS1R	AR	NM_032551.5:c.581C > A	p.Ala194Asp	Heterozygous	VUS	0.000352	0.000882	0.977	Boehm et al. (2015)	Miraoui et al. (2013)
36	M	pubertal delay	MASTL	AD, di-, trigenic (Quaynor et al. 2016)	NM_001172303.2:c.1505A > G	p.Asp502Gly	Heterozygous	VUS	Absent	Absent	0.9219	Quaynor et al. (2016)	Novel in IHH
37	M	pubertal delay	SPRY4	AD	NM_030964.3:c.626G > A	p.Cys209Tyr	Heterozygous	VUS^b	0.002170	0.003450	0.9971	Miraoui et al. (2013)	HGMD ID: CM133832 Miraoui et al. (2013)
37	M	pubertal delay	AMH	AR (Malone et al. 2019)	NM_000479.4:c.761G > C	p.Arg254Pro	Heterozygous	VUS^b	0.000015	0.000000	0.9626	Malone et al. (2019)	Novel in IHH
39	M	KS	FGFR1	AD, contributes to oligogenicity	NM_001174067.1:c.367G>T	p.Asp123Tyr	Heterozygous	VUS	0.000059	0.000000	0.9944	Boehm et al. (2015)	Novel in IHH (It was reported in deafness variation database https://deafnessvariationdatabase.org/)
39	M	KS	GLI3	digenic (Quaynor et al. 2016)	NM_000168.6:c.1163C > T	p.Pro388Leu	Heterozygous	VUS	Absent	Absent	0.7657	Quaynor et al. (2016)	Novel in IHH
40	M	KS	FGFR1	AD, contributes to oligogenicity	NM_001174067.1:c.550C > A	p.Pro184Thr	Heterozygous	VUS	Absent	Absent	0.9974	Boehm et al. (2015)	Novel in IHH

Gene references:

Boehm et al. (2015), Malone et al. (2019), Quaynor et al. (2016)

Variant references:

Dodé et al. (2006), Cole et al. (2008), Monnier et al. (2009), Abreu et al. (2010), Reynaud et al. (2012), Cassatella et al. (2018), Amato et al. (2019), Hughes et al. (2019), Costa et al. (2001), Topaloglu et al. (2006), Beneduzzi et al. (2014), Radhakrishna et al. (1999), Gürbüz et al. (2012), Digilio et al. (2019), Tommiska et al. (2013), Tusset et al. (2012), Miraoui et al. (2013)

^aAfter family screening, we considered this variant not disease causing as the unaffected father carried the same variant in heterozygous form

^bAfter family screening, we considered these variants not disease causing as the unaffected father carried both variants in heterozygous form